Document:

EX-4.2

Exhibit 4.2

Consolidated Financial Statements of

THERATECHNOLOGIES INC.

Years ended November 30, 2010 and 2009 and as at December 1, 2008

 

 

	 	 	 	 	 

	KPMG LLP

	 	Telephone
	 	(514) 840-2100
	Chartered Accountants

	 	Fax
	 	(514) 840-2187
	600 de Maisonneuve Blvd. West

	 	Internet
	 	www.kpmg.ca
	Suite 1500
	 	 	 	 
	Tour KPMG
	 	 	 	 
	Montréal (Québec) H3A 03A
	 	 	 	 

AUDITORS’ REPORT TO THE SHAREHOLDERS

We have audited the consolidated statements of financial position of Theratechnologies Inc. as
at November 30, 2010 and 2009 and December 1, 2008, and the consolidated statements of
comprehensive income, statements of changes in equity and statements of cash flows for the years
ended November 30, 2010 and 2009. These financial statements are the responsibility of the
Company’s management. Our responsibility is to express an opinion on these financial statements
based on our audits.

We conducted our audits in accordance with Canadian generally accepted auditing standards. Those
standards require that we plan and perform an audit to obtain reasonable assurance whether the
financial statements are free of material misstatement. An audit includes examining, on a test
basis, evidence supporting the amounts and disclosures in the financial statements. An audit also
includes assessing the accounting principles used and significant estimates made by management, as
well as evaluating the overall financial statement presentation.

In our opinion, these consolidated financial statements present fairly, in all material respects,
the financial position of the Company as at November 30, 2010 and 2009 and December 1, 2008, and
its financial performance and its cash flows for the years ended November 30, 2010 and 2009 in
accordance with International Financial Reporting Standards as issued by the International
Accounting Standards Board.

Chartered Accountants

Montréal, Canada

February 8, 2011

*CA Auditor permit no 14553

KPMG LLP is a Canadian limited liability partnership and a member firm of the KPMG

network of independent member firms affiliated with KPMG International Cooperative

(“KPMG International”), a Swiss entity.

KPMG Canada provides services to KPMG LLP.

 

 

THERATECHNOLOGIES INC.

Consolidated Financial Statements

Years ended November 30, 2010 and 2009 and as at December 1, 2008

Financial Statements

	 	 	 	 	 

	Consolidated Statement of Financial Position
	 	 	1	 
	Consolidated Statement of Comprehensive Income
	 	 	2	 
	Consolidated Statement of Changes in Equity
	 	 	3	 
	Consolidated Statement of Cash Flows
	 	 	4	 
	Notes to the Consolidated Financial Statements
	 	 	5	 

 

 

THERATECHNOLOGIES INC.

Consolidated Statement of Financial Position

As at November 30, 2010 and 2009 and December 1, 2008

(in thousands of Canadian dollars)
 

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	November 30,	 	 	November 30,	 	 	December 1,	 
	 	 	Note	 	 	2010	 	 	2009	 	 	2008	 
	 	 	 	 	 	 	$	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Assets
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Current assets:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Cash
	 	 	 	 	 	 	26,649	 	 	 	1,519	 	 	 	133	 
	Bonds
	 	 	8	 	 	 	1,860	 	 	 	10,036	 	 	 	10,955	 
	Trade and other receivables
	 	 	9	 	 	 	161	 	 	 	375	 	 	 	610	 
	Tax credits and grants receivable
	 	 	10	 	 	 	332	 	 	 	1,333	 	 	 	1,451	 
	Inventories
	 	 	11	 	 	 	4,317	 	 	 	2,225	 	 	 	—	 
	Prepaid expenses
	 	 	 	 	 	 	1,231	 	 	 	630	 	 	 	739	 
	 
	Total current assets
	 	 	 	 	 	 	34,550	 	 	 	16,118	 	 	 	13,888	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Non-current assets:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Bonds
	 	 	8	 	 	 	36,041	 	 	 	51,807	 	 	 	35,249	 
	Property and equipment
	 	 	12	 	 	 	1,060	 	 	 	1,229	 	 	 	1,299	 
	Other assets
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	2,776	 
	 
	Total non-current assets
	 	 	 	 	 	 	37,101	 	 	 	53,036	 	 	 	39,324	 
	 
	Total assets
	 	 	 	 	 	 	71,651	 	 	 	69,154	 	 	 	53,212	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Liabilities
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Current liabilities:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Accounts payable and accrued liabilities
	 	 	13	 	 	 	4,977	 	 	 	5,568	 	 	 	6,865	 
	Current portion of deferred revenue
	 	 	4	 	 	 	6,847	 	 	 	6,847	 	 	 	—	 
	 
	Total current liabilities
	 	 	 	 	 	 	11,824	 	 	 	12,415	 	 	 	6,865	 
	 
	Non-current liabilities:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Other liabilities
	 	 	14	 	 	 	325	 	 	 	—	 	 	 	—	 
	Deferred revenue
	 	 	4	 	 	 	6,846	 	 	 	13,691	 	 	 	—	 
	 
	Total non-current liabilities
	 	 	 	 	 	 	7,171	 	 	 	13,691	 	 	 	—	 
	 
	Total liabilities
	 	 	 	 	 	 	18,995	 	 	 	26,106	 	 	 	6,865	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Equity
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Share capital
	 	 	15	 	 	 	279,398	 	 	 	279,169	 	 	 	269,219	 
	Contributed surplus
	 	 	 	 	 	 	7,808	 	 	 	6,757	 	 	 	5,760	 
	Deficit
	 	 	 	 	 	 	(235,116	)	 	 	(244,160	)	 	 	(229,004	)
	Accumulated other comprehensive income
	 	 	 	 	 	 	566	 	 	 	1,282	 	 	 	372	 
	 
	Total equity
	 	 	 	 	 	 	52,656	 	 	 	43,048	 	 	 	46,347	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Contingent liability
	 	 	18	 	 	 	 	 	 	 	 	 	 	 	 	 
	Commitments
	 	 	23	 	 	 	 	 	 	 	 	 	 	 	 	 
	Subsequent events
	 	 	26	 	 	 	 	 	 	 	 	 	 	 	 	 
	 
	Total liabilities and equity
	 	 	 	 	 	 	71,651	 	 	 	69,154	 	 	 	53,212	 
	 

See accompanying notes to the consolidated financial statements.

	 	 	 

	On behalf of the Board,
	 	 
	 
	 	 
	(signed) Paul Pommier

	 	(signed) Jean-Denis Talon
	 

	 	 
	Director

	 	Director

1

 

THERATECHNOLOGIES INC.

Consolidated Statement of Comprehensive Income

Years ended November 30, 2010 and 2009

(in thousands of Canadian dollars, except per share amounts)

 

	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	November 30,	 	 	November 30,	 
	 	 	Note	 	 	2010	 	 	2009	 
	 
	 	 	 	 	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Revenue:
	 	 	 	 	 	 	 	 	 	 	 	 
	Research services:
	 	 	 	 	 	 	 	 	 	 	 	 
	Milestone payments
	 	 	4	 	 	 	25,000	 	 	 	10,884	 
	Upfront payments and initial technology access fees
	 	 	4	 	 	 	6,846	 	 	 	6,560	 
	Royalties and license fees
	 	 	 	 	 	 	22	 	 	 	24	 
	 
	Total revenue
	 	 	 	 	 	 	31,868	 	 	 	17,468	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Cost of sales
	 	 	 	 	 	 	469	 	 	 	—	 
	Research and development expenses, net of tax credits of $934 (2009 - $1,795)
	 	 	10	 	 	 	14,064	 	 	 	20,810	 
	Selling and market development expenses
	 	 	6	 	 	 	2,670	 	 	 	6,862	 
	General and administrative expenses
	 	 	 	 	 	 	8,002	 	 	 	6,543	 
	 
	Total operating expenses
	 	 	 	 	 	 	25,205	 	 	 	34,215	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Results from operating activities
	 	 	 	 	 	 	6,663	 	 	 	(16,747	)
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Finance income
	 	 	7	 	 	 	1,888	 	 	 	2,252	 
	Finance costs
	 	 	7	 	 	 	493	 	 	 	(661	)
	 
	Total net financial income
	 	 	 	 	 	 	2,381	 	 	 	1,591	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Net profit (loss) before income taxes
	 	 	 	 	 	 	9,044	 	 	 	(15,156	)
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Income tax expense
	 	 	16	 	 	 	114	 	 	 	—	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	 
	Net profit (loss)
	 	 	 	 	 	 	8,930	 	 	 	(15,156	)
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Other comprehensive income (loss), net of tax:
	 	 	 	 	 	 	 	 	 	 	 	 
	Net change in fair value available-for-sale financial assets, net of tax
	 	 	 	 	 	 	(390	)	 	 	1,039	 
	Net change in fair value available-for-sale financial assets transferred to net profit (loss),
net of tax
	 	 	 	 	 	 	(326	)	 	 	(129	)
	 
	 
	 	 	 	 	 	 	(716	)	 	 	910	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	 
	Total comprehensive income (loss) for the year
	 	 	 	 	 	 	8,214	 	 	 	(14,246	)
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Basic and diluted earnings (loss) per share
	 	 	15	 	 	 	0.15	 	 	 	(0.25	)
	 

See accompanying notes to the consolidated financial statements.

2

 

THERATECHNOLOGIES INC.

Consolidated Statement of Changes in Equity

Years ended November 30, 2010 and 2009

(in thousands of Canadian dollars)

 

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	Unrealized gains	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	or losses on	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	available-for-sale	 	 	 	 	 	 	 
	 	 	 	 	 	 	Share capital	 	 	Contributed	 	 	financial	 	 	 	 	 	 	 
	 	 	Note	 	 	Number	 	 	Dollars	 	 	surplus	 	 	assets (i)	 	 	Deficit	 	 	Total	 
	 
	 	 	 	 	 	 	 	 	 	 	$	 	 	$	 	 	$	 	 	$	 	 	$	 
	Balance as at December 1, 2008
	 	 	 	 	 	 	58,215,090	 	 	 	269,219	 	 	 	5,760	 	 	 	372	 	 	 	(229,004	)	 	 	46,347	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Total comprehensive income (loss) for the year:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Net loss
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	(15,156	)	 	 	(15,156	)
	Other comprehensive income (loss):
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Net change in fair value of available-for-sale financial assets, net of tax
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	1,039	 	 	 	—	 	 	 	1,039	 
	Net change in fair value of available-for-sale financial assets transferred to net profit (loss),
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	net of tax
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	(129	)	 	 	—	 	 	 	(129	)
	 
	Total comprehensive income (loss) for the year
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	910	 	 	 	(15,156	)	 	 	(14,246	)
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Transactions with owners, recorded directly in equity:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Issue of common shares
	 	 	15 	(i)	 	 	2,214,303	 	 	 	9,950	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	9,950	 
	Share-based compensation for stock option plan
	 	15 (iv)	 	 	—	 	 	 	—	 	 	 	997	 	 	 	—	 	 	 	—	 	 	 	997	 
	 
	Total contributions by owners
	 	 	 	 	 	 	2,214,303	 	 	 	9,950	 	 	 	997	 	 	 	—	 	 	 	—	 	 	 	10,947	 
	 
	Balance as at November 30, 2009
	 	 	 	 	 	 	60,429,393	 	 	 	279,169	 	 	 	6,757	 	 	 	1,282	 	 	 	(244,160	)	 	 	43,048	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Total comprehensive income (loss) for the year:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Net profit
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	8,930	 	 	 	8,930	 
	Other comprehensive income (loss):
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Net change in fair value of available-for-sale financial assets, net of tax
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	(390	)	 	 	—	 	 	 	(390	)
	Net change in fair value of available-for-sale financial assets transferred to net profit (loss),
net of tax
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	(326	)	 	 	—	 	 	 	(326	)
	 
	Total comprehensive income (loss) for the year
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	(716	)	 	 	8,930	 	 	 	8,214	 
	 
	Transactions with owners, recorded directly in equity:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Issue of common shares
	 	 	15 	(i)	 	 	2,880	 	 	 	15	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	15	 
	Income tax related to share issue costs
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	114	 	 	 	114	 
	Share-based compensation plan:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Share-based compensation for stock option plan
	 	15 (iv)	 	 	—	 	 	 	—	 	 	 	1,133	 	 	 	—	 	 	 	—	 	 	 	1,133	 
	Exercise of stock options:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Monetary consideration
	 	15 (iv)	 	 	80,491	 	 	 	132	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	132	 
	Attributed value
	 	15 (iv)	 	 	—	 	 	 	82	 	 	 	(82	)	 	 	—	 	 	 	—	 	 	 	—	 
	 
	Total contributions by owners
	 	 	 	 	 	 	83,371	 	 	 	229	 	 	 	1,051	 	 	 	—	 	 	 	114	 	 	 	1,394	 
	 
	Balance as at November 30, 2010
	 	 	 	 	 	 	60,512,764	 	 	 	279,398	 	 	 	7,808	 	 	 	566	 	 	 	(235,116	)	 	 	52,656	 
	 

 

			
	(i)	 	Accumulated other comprehensive income.

See accompanying notes to the consolidated financial statements.

3

 

THERATECHNOLOGIES INC.

Consolidated Statement of Cash Flows

Years ended November 30, 2010 and 2009

(in thousands of Canadian dollars)

 

	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	November 30,	 	 	November 30,	 
	 	 	Note	 	 	2010	 	 	2009	 
	 
	 	 	 	 	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Operating activities:
	 	 	 	 	 	 	 	 	 	 	 	 
	Net profit (loss)
	 	 	 	 	 	 	8,930	 	 	 	(15,156	)
	Adjustments for:
	 	 	 	 	 	 	 	 	 	 	 	 
	Depreciation of property and equipment
	 	 	12	 	 	 	466	 	 	 	612	 
	Share-based compensation
	 	 	 	 	 	 	1,133	 	 	 	997	 
	Income tax expense
	 	 	 	 	 	 	114	 	 	 	—	 
	Write-down of inventories
	 	 	11	 	 	 	192	 	 	 	—	 
	Lease inducements and amortization
	 	 	17	 	 	 	325	 	 	 	—	 
	 
	Operating activities before changes in operating assets and liabilities
	 	 	 	 	 	 	11,160	 	 	 	(13,547	)
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Change in accrued interest income on bonds
	 	 	 	 	 	 	728	 	 	 	(923	)
	Change in trade and other receivables
	 	 	 	 	 	 	214	 	 	 	235	 
	Change in tax credits and grants receivable
	 	 	 	 	 	 	1,001	 	 	 	118	 
	Change in inventories
	 	 	 	 	 	 	(2,284	)	 	 	(2,225	)
	Change in prepaid expenses
	 	 	 	 	 	 	(601	)	 	 	109	 
	Change in other assets
	 	 	 	 	 	 	—	 	 	 	2,776	 
	Change in accounts payable and accrued liabilities
	 	 	 	 	 	 	(473	)	 	 	(1,424	)
	Change in deferred revenue
	 	 	 	 	 	 	(6,845	)	 	 	20,538	 
	 
	 
	 	 	 	 	 	 	(8,260	)	 	 	19,204	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	 
	Cash flows from operating activities
	 	 	 	 	 	 	2,900	 	 	 	5,657	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Financing activities:
	 	 	 	 	 	 	 	 	 	 	 	 
	Proceeds from issue of share capital
	 	 	 	 	 	 	15	 	 	 	9,950	 
	Proceeds from exercise of stock options
	 	 	15	 	 	 	132	 	 	 	—	 
	Share issue costs
	 	 	 	 	 	 	—	 	 	 	(8	)
	 
	Cash flows from financing activities
	 	 	 	 	 	 	147	 	 	 	9,942	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Investing activities:
	 	 	 	 	 	 	 	 	 	 	 	 
	Acquisition of property and equipment
	 	 	12	 	 	 	(415	)	 	 	(407	)
	Proceeds from sale of bonds
	 	 	 	 	 	 	22,498	 	 	 	15,305	 
	Acquisition of bonds
	 	 	 	 	 	 	—	 	 	 	(29,111	)
	 
	Cash flows from (used in) investing activities
	 	 	 	 	 	 	22,083	 	 	 	(14,213	)
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	 
	Net change in cash
	 	 	 	 	 	 	25,130	 	 	 	1,386	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Cash as at December 1
	 	 	 	 	 	 	1,519	 	 	 	133	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	 
	Cash as at November 30
	 	 	 	 	 	 	26,649	 	 	 	1,519	 
	 

See note 19 for supplemental cash flow information.

See accompanying notes to the consolidated financial statements.

4

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in
thousands of Canadian dollars, except per share amounts)

 

	1.	 	Reporting entity:
	 
	 	 	Theratechnologies Inc. is a specialty pharmaceutical company that discovers and develops
innovative therapeutic peptide products with an emphasis on growth hormone releasing factor
peptides. Theratechnologies Inc. is leveraging its expertise in the field of metabolism to
discover and develop products in specialty markets. Its commercialization strategy is to retain
all or a significant portion of the commercial rights to its products. Its first product,
EGRIFTATM (tesamorelin for injection), was approved by the United States
Food and Drug Administration (“FDA”) in November 2010. To date,
EGRIFTATM is the only approved therapy for the reduction of excess
abdominal fat in HIV-infected patients with lipodystrophy.
	 
	 	 	The consolidated financial statements include the accounts of Theratechnologies Inc. and its
wholly-owned subsidiaries (together referred to as the “Company” and individually as “the
subsidiaries of the Company”).
	 
	 	 	Theratechnologies Inc. is incorporated under Part 1A of the Québec Companies Act and is
domiciled in Quebec, Canada. The Company is located at 2310 boul. Alfred-Nobel, Montreal,
Quebec, H4S 2B4.
	 
	2.	 	Basis of preparation:

	 	(a)	 	Statement of compliance:
	 
	 	 	 	The consolidated financial statements of the Company have been prepared in accordance with
IFRSs as issued by the International Accounting Standards Board (“IASB”). These are the
Company’s first consolidated financial statements prepared in accordance with International
Financial Reporting Standards (“IFRSs”). The Company has applied IFRS 1,
First-time Adoption of International Financial Reporting Standards, using December 1, 2008
as the date of transition to IFRSs.
	 
	 	 	 	An explanation of how the transition to IFRSs has affected the reported financial position,
financial performance and cash flows of the Company is provided in note 27.
	 
	 	 	 	The consolidated financial statements were authorized for issue by the Board of Directors
on February 8, 2011.
	 
	 	(b)	 	Basis of measurement:
	 
	 	 	 	The Company’s consolidated financial statements have been prepared on a going concern and
historical cost basis, except for available-for-sale financial assets which are measured at
fair value.
	 
	 	 	 	The methods used to measure fair value are discussed further in note 22.

5

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
(in
thousands of Canadian dollars, except per share amounts)

 

	2.	 	Basis of preparation (continued):

	 	(c)	 	Functional and presentation currency:
	 
	 	 	 	These consolidated financial statements are presented in Canadian dollars, which is the
Company’s functional currency. All financial information presented in Canadian dollars has
been rounded to the nearest thousand.
	 
	 	(d)	 	Use of estimates and judgements:
	 
	 	 	 	The preparation of the Company’s consolidated financial statements in conformity with IFRSs
requires management to make estimates and assumptions that affect the reported amounts of
assets and liabilities and disclosure of contingent assets and liabilities at the date of
the financial statements and the reported amounts of revenues and expenses during the
reporting period.
	 
	 	 	 	Information about critical judgements in applying accounting policies and assumption and
estimation uncertainties that have the most significant effect on the amounts recognized in
the consolidated financial statements is included in the following notes:

	 	•	 	Note 4 — Revenue and deferred revenue;
	 
	 	•	 	Note 15 (iv) — Stock option plan;
	 
	 	•	 	Note 16 — Income taxes;
	 
	 	•	 	Note 18 — Contingent liability.

	 	 	 	Other areas of judgement and uncertainty relate to the estimation of accruals for clinical
trial expenses, the recoverability of inventories, the measurement of the amount and
assessment of the recoverability of tax credits and grants receivable and capitalization of
development expenditures.
	 
	 	 	 	Reported amounts and note disclosure reflect the overall economic conditions that are most
likely to occur and anticipated measures management intends to take. Actual results could
differ from those estimates.
	 
	 	 	 	The above estimates and assumptions are reviewed regularly. Revisions to accounting
estimates are recognized in the period in which the estimates are revised and in any future
periods affected.

	3.	 	Significant accounting policies:
	 
	 	 	The accounting policies set out below have been applied consistently to all periods presented
in these consolidated financial statements and in preparing the opening IFRS statement of
financial position at December 1, 2008, the date of transition to IFRSs.

6

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
(in
thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):
	 
	 	 	The accounting policies have been applied consistently by the subsidiaries of the Company.

	 	(a)	 	Basis of consolidation:
	 
	 	 	 	The financial statements of subsidiaries are included in the consolidated financial
statements from the date on which control commences until the date on which control ceases.
Subsidiaries are entities controlled by the Company. Control is present where the Company
has the power to govern the financial and operating policies of the entity so as to obtain
benefits from its activities. In assessing control, potential voting rights that are
exercisable currently are taken into consideration. The accounting policies of subsidiaries
are changed when necessary to align them with the policies adopted by the Company.
	 
	 	 	 	Reciprocal balances and transactions, revenues and expenses resulting from transactions
between subsidiaries and with the Company are eliminated in preparing the consolidated
financial statements.
	 
	 	(b)	 	Foreign currency:
	 
	 	 	 	Transactions in foreign currencies are translated to the respective functional currencies
of the subsidiaries of the Company at exchange rates at the dates of the transactions.
Monetary assets and liabilities denominated in foreign currencies at the reporting date are
retranslated to the functional currency at the exchange rate at that date. The foreign
currency gain or loss on monetary items is the difference between amortized cost in the
functional currency at the beginning of the period, adjusted for effective interest and
payments during the period, and the amortized cost in foreign currency translated at the
exchange rate at the end of the reporting period.
	 
	 	 	 	Foreign currency differences arising on translation are recognized in net profit (loss),
except for differences arising on the translation of available-for-sale equity instruments,
which are recognized in other comprehensive income. Non-monetary assets and liabilities
denominated in foreign currencies that are measured at fair value are translated to the
functional currency at the exchange rate at the date on which the fair value was
determined. Non-monetary items that are measured at historical cost in a foreign currency
are translated using the exchange rate at the date of the transaction.
	 
	 	(c)	 	Revenue recognition:
	 
	 	 	 	Collaboration agreements that include multiple deliverables are considered to be
multi-element arrangements. Under this type of arrangement, the identification of separate
units of accounting is required and revenue is allocated among the separate units based on
their relative fair values.

7

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
(in
thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(c)	 	Revenue recognition (continued):
	 
	 	 	 	Payments received under the collaboration agreement may include upfront payments, milestone
payments, research services, royalties and license fees. Revenues for each unit of
accounting are recorded as described below:

	 	(i)	 	Sale of goods:
	 
	 	 	 	Revenues from the sale of goods are recognized when the Company has transferred to the
buyer the significant risks and rewards of ownership of the goods, there is no
continuing management involvement with the goods, and the amount of revenue can be
measured reliably.
	 
	 	(ii)	 	Royalties and license fees:
	 
	 	 	 	Royalties and license fees are recognized when conditions and events under the license
agreement have occurred and collectibility is reasonably assured.
	 
	 	(iii)	 	Research services:
	 
	 	 	 	Revenues from research contracts are recognized when services to be provided are
rendered and all conditions under the terms of the underlying agreement are met.

	 	(a)	 	Upfront payments and initial technology access fees:
	 
	 	 	 	Upfront payments and initial technology access fees are deferred and recognized as
revenue on a systematic basis over the period during which the related products or
services are delivered and all obligations are performed.
	 
	 	(b)	 	Milestone payments:
	 
	 	 	 	Revenues subject to the achievement of milestones are recognized only when the
specified events have occurred and collectibility is reasonably assured.

	 	(d)	 	Cost of sales:
	 
	 	 	 	Cost of sales represents the cost of goods sold and includes the cost of raw materials,
supplies, direct overhead charges, unallocated indirect costs related to production as well
as write-down of inventories. Other direct costs, such as manufacturing start-up costs
between validation and the achievement of normal production, are expensed as incurred.

8

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
(in
thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(e)	 	Employee benefits:
	 
	 	 	 	Salaries and short-term employee benefits:
	 
	 	 	 	Salaries and short-term employee benefit obligations are measured on an undiscounted basis
and are expensed as the related service is provided. A liability is recognized for the
amount expected to be paid under short-term profit-sharing or cash bonus plans if the
Company has a legal or constructive obligation to pay an amount as a result of past
services rendered by an employee and the obligation can be estimated reliably.
	 
	 	 	 	Post-employment benefits:
	 
	 	 	 	Post-employment benefits include a defined contribution plan under which an entity pays
fixed contributions into a separate entity and will have no legal or constructive
obligation to pay further amounts. Obligations for contributions to defined contribution
plans are recognized as an employee benefit expense when due. Prepaid contributions are
recognized as an asset to the extent that a cash refund or a reduction in future payments
is available. The Company’s defined contribution plan comprises the registered retirement
savings plan, the Quebec Pension Plan and unemployment insurance.
	 
	 	 	 	Termination benefits:
	 
	 	 	 	Termination benefits are recognized as an expense when the Company is committed
demonstrably, without realistic possibility of withdrawal, to a formal detailed plan to
either terminate employment before the normal retirement date, or to provide termination
benefits as a result of an offer made to encourage voluntary redundancy.
	 
	 	(f)	 	Finance income and finance costs:
	 
	 	 	 	Finance income comprises interest income on available-for-sale financial assets and gains
(losses) on the disposal of available-for-sale financial assets. Interest income is
recognized as it accrues in profit (loss), using the effective interest method.
	 
	 	 	 	Finance costs are comprised of bank charges, impairment losses on financial assets
recognized in profit (loss) and of foreign currency gains and losses which are reported on
a net basis.

9

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
(in
thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(g)	 	Inventories:
	 
	 	 	 	Inventories are presented at the lower of cost, determined using the first-in first-out
method, or net realizable value. Inventory costs include the purchase price and other costs
directly related to the acquisition of materials, and other costs incurred in bringing the
inventories to their present location and condition. Inventory costs also include the costs
directly related to the conversion of materials to finished goods, such as direct labour,
and a systematic allocation of fixed and variable production overhead, including
manufacturing depreciation expense. The allocation of fixed production overheads to the
cost of inventories is based on the normal capacity of the production facilities. Normal
capacity is the average production expected to be achieved over a number of periods under
normal circumstances.
	 
	 	 	 	Net realizable value is the estimated selling price in the Company’s ordinary course of
business, less the estimated costs of completion and selling expenses.
	 
	 	(h)	 	Property and equipment:
	 
	 	 	 	Recognition and measurement:
	 
	 	 	 	Items of property and equipment are recognized at cost less accumulated depreciation and
accumulated impairment losses. Cost includes expenditure that is directly attributable to
the acquisition of the asset and the costs of dismantling and removing the item and
restoring the site on which it is located, if any.
	 
	 	 	 	When parts of an item of property and equipment have different useful lives, they are
accounted for as separate items (major components) of property and equipment.
	 
	 	 	 	Gains and losses on disposal of an item of property and equipment are determined by
comparing the proceeds from disposal with the carrying amount of property and equipment,
and are recognized in net profit (loss).
	 
	 	 	 	Subsequent costs:
	 
	 	 	 	The cost of replacing a part of an item of property and equipment is recognized in the
carrying amount of the item if it is probable that the future economic benefits embodied
within the part will flow to the Company, and its cost can be measured reliably. The
carrying amount of the replaced part is derecognized. The costs of the day-to-day servicing
of property and equipment are recognized in profit (loss) as incurred.

10

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
 (in
thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(h)	 	Property and equipment (continued):
	 
	 	 	 	Depreciation:
	 
	 	 	 	The estimated useful lives and the methods of depreciation for the current and comparative
periods are as follows:

	 	 	 	 	 	 	 
	Asset	 	Method	 	Rate/Period	 
	 
	Computer equipment

	 	Declining balance
	 	 	50	%
	Laboratory equipment

	 	Declining balance
	 	 	20	%
	 

	 	and straight-line
	 	 	5 years
	 
	Office furniture and equipment

	 	Declining balance
	 	 	20	%
	Leasehold improvements

	 	Straight-line
	 	 	Lower of term of lease
or economic life
	 

	 	 	 	This most closely reflects the expected pattern of consumption of the future economic
benefits embodied in the asset.
	 
	 	 	 	Estimates for depreciation methods, useful lives and residual values are reviewed at each
reporting period-end and adjusted if appropriate.
	 
	 	(i)	 	Intangible assets:
	 
	 	 	 	Research and development:
	 
	 	 	 	Expenditure on research activities, undertaken with the prospect of gaining new scientific
or technical knowledge and understanding, is expensed as incurred.
	 
	 	 	 	Development activities involve a plan or design for the production of new or substantially
improved products and processes. Development expenditure is capitalized only if development
costs can be measured reliably, the product or process is technically and commercially
feasible, future economic benefits are probable, and the Company intends to and has
sufficient resources to complete development and to use or sell the asset. These criteria
are usually met when a regulatory filing has been made in a major market and approval is
considered highly probable. The expenditure capitalized includes the cost of materials,
direct labour, and overhead costs that are directly attributable to preparing the asset for
its intended use. Other development expenditures are expensed as incurred. Capitalized
development expenditures are measured at cost less accumulated amortization and accumulated
impairment losses.
	 
	 	 	 	During the years ended November 30, 2010 and 2009 and as at December 1, 2008, no
development expenditures were capitalized.

11

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
 (in
thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(j)	 	Financial instruments:
	 
	 	 	 	The Company’s financial instruments are classified into one of three categories: loans and
receivables, available-for-sale financial assets and other financial liabilities. Loans and
receivables and other financial liabilities are measured at amortized cost.
	 
	 	 	 	The Company has classified its bonds as available-for-sale financial assets. The Company
has classified cash and trade and other receivables as loans and receivables, and accounts
payable and accrued liabilities as other financial liabilities.
	 
	 	 	 	Available-for-sale financial assets are non-derivative financial assets that are designated
as available-for-sale and that are not classified in any of the other categories.
Subsequent to initial recognition, they are measured at fair value and changes therein,
other than impairment losses and foreign currency differences on available-for-sale debt
instruments, are recognized in other comprehensive income and presented within equity. When
an investment is derecognized, the cumulative gain or loss in other comprehensive income is
transferred to profit (loss).
	 
	 	(k)	 	Other assets:
	 
	 	 	 	Other assets consist of prepaid expenses for research supplies that are not expected to be
used within one year from the date of the consolidated statement of financial position.
	 
	 	 	 	Research supplies are purchased in advance, in accordance with specific regulatory
requirements, to be used in connection with the Company’s clinical trials.
	 
	 	(l)	 	Leases:
	 
	 	 	 	Operating lease payments are recognized in net profit (loss) on a straight-line basis over
the term of the lease.
	 
	 	 	 	Lease inducements arising from leasehold improvement allowances and rent-free periods form
an integral part of the total lease cost and are deferred and recognized in net profit
(loss) over the term of the lease on a straight-line basis.

12

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
 (in
thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(m)	 	Impairment:
	 
	 	 	 	Financial assets:
	 
	 	 	 	A financial asset not carried at fair value through profit or loss is assessed at each
consolidated financial statement reporting date to determine whether there is objective
evidence that it is impaired. The Company considers that a financial asset is impaired if
objective evidence indicates that one or more loss events had a negative effect on the
estimated future cash flows of that asset that can be estimated reliably.
	 
	 	 	 	An impairment test is performed, on an individual basis, for each material financial asset.
Other individually non-material financial assets are tested as groups of financial assets
with similar risk characteristics. Impairment losses are recognized in net profit (loss).
	 
	 	 	 	An impairment loss in respect of a financial asset measured at amortized cost is calculated
as the difference between its carrying amount and the present value of the estimated future
cash flows discounted at the asset’s original effective interest rate. Losses are
recognized in net profit (loss) and reflected in an allowance account against the
respective financial asset. Interest on the impaired asset continues to be recognized
through the unwinding of the discount. When a subsequent event causes the amount of
impairment loss to decrease, the decrease in impairment loss is reversed through net profit
(loss).
	 
	 	 	 	Impairment losses on available-for-sale investment securities are recognized by
transferring the cumulative loss that has been recognized in other comprehensive income,
and presented in unrealized gains/losses on available-for-sale financial assets in equity,
to net profit (loss). The cumulative loss that is removed from other comprehensive income
and recognized in net profit (loss) is the difference between the acquisition cost, net of
any principal repayment and amortization, and the current fair value, less any impairment
loss previously recognized in net profit (loss). Changes in impairment provisions
attributable to time value are reflected as a separate component of interest income.
	 
	 	 	 	If, in a subsequent period, the fair value of an impaired available-for-sale debt security
increases and the increase can be related objectively to an event occurring after the
impairment loss was recognized in net profit (loss), then the impairment loss is reversed,
with the amount of the reversal recognized in net profit (loss). However, any subsequent
recovery in the fair value of an impaired available-for-sale equity security is recognized
in other comprehensive income.

13

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
 (in
thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(m)	 	Impairment (continued):
	 
	 	 	 	Non-financial assets:
	 
	 	 	 	The carrying amounts of the Company’s non-financial assets, other than inventories and
deferred tax assets, are reviewed at each reporting date to determine whether there is any
indication of impairment. If such an indication exists, the recoverable amount is
estimated.
	 
	 	 	 	The recoverable amount of an asset or a cash-generating unit is the greater of its value in
use and its fair value less costs to sell. In assessing value in use, the estimated future
cash flows are discounted to their present value using a pre-tax discount rate that
reflects current market assessments of the time value of money and the risks specific to
the asset. For the purpose of impairment testing, assets are grouped together into the
smallest group of assets that generates cash inflows from continuing use that are largely
independent of cash inflows from other assets or groups of assets (''cash-generating
unit’’). Impairment losses recognized in prior periods are determined at each reporting
date for any indications that the loss has decreased or no longer exists. An impairment
loss is reversed if there has been a change in the estimates used to determine the
recoverable amount. An asset’s carrying amount, increased through reversal of an impairment
loss, must not exceed the carrying amount that would have been determined, net of
depreciation or amortization, if no impairment loss had been recognized.
	 
	 	(n)	 	Provisions:
	 
	 	 	 	A provision is recognized if, as a result of a past event, the Company has a present legal
or constructive obligation that can be estimated reliably, and it is probable that an
outflow of economic benefits will be required to settle the obligation. Provisions are
assessed by discounting the expected future cash flows at a pre-tax rate that reflects
current market assessments of the time value of money and the risks specific to the
liability. The unwinding of the discount on provisions is recognized in finance costs.
	 
	 	 	 	Onerous contracts:
	 
	 	 	 	A provision for onerous contracts is recognized when the expected benefits to be derived by
the Company from a contract are lower than the unavoidable cost of meeting its obligations
under the contract. The provision is measured at the present value of the lower of the
expected cost of terminating the contract and the expected net cost of continuing with the
contract. Before a provision is established, the Company recognizes any impairment loss on
the assets associated with that contract. There were no onerous contracts as at November
30, 2010 and 2009 and December 1, 2008.

14

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
 (in
thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(n)	 	Provisions (continued):
	 
	 	 	 	Site restoration:
	 
	 	 	 	Where there is a legal or constructive obligation to restore leased premises to good
condition, except for normal aging on expiry or early termination of the lease, the
resulting costs are provisioned up to the discounted value of estimated future costs and
increase the carrying amount of the corresponding item of property and equipment. The
Company amortizes the cost of restoring leased premises and recognizes an unwinding of
discount expense on the liability related to the term of the lease.
	 
	 	 	 	Contingent liability:
	 
	 	 	 	A contingent liability is a possible obligation that arises from past events and of which
the existence will be confirmed only by the occurrence or non-occurrence of one or more
uncertain future events not wholly within the control of the Company; or a present
obligation that arises from past events (and therefore exists), but is not recognized
because it is not probable that a transfer or use of assets, provision of services or any
other transfer of economic benefits will be required to settle the obligation, or the
amount of the obligation cannot be estimated reliably.
	 
	 	(o)	 	Income taxes:
	 
	 	 	 	Income tax expense comprises current and deferred tax. Current tax and deferred tax are
recognized in net profit (loss) except to the extent that they relate to items recognized
directly in other comprehensive income or in equity.
	 
	 	 	 	Current tax:
	 
	 	 	 	Current tax is the expected tax payable or receivable on the taxable income or loss for the
year, using tax rates enacted or substantively enacted at the reporting date, and any
adjustment to tax payable in respect of previous years. The Company establishes provisions
where appropriate on the basis of amounts expected to be paid to the tax authorities.
	 
	 	 	 	Deferred tax:
	 
	 	 	 	Deferred tax is recognized in respect of temporary differences between the carrying amounts
of assets and liabilities for financial reporting purposes and the amounts used for
taxation purposes. Deferred tax is measured at the tax rates that are expected to be
applied to temporary differences when they reverse, based on the laws that have been
enacted or substantively enacted by the reporting date.
	 
	 	 	 	A deferred tax liability is generally recognized for all taxable temporary differences.

15

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008
 (in
thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(o)	 	Income taxes
(continued): 
	 
	 	 	 	 Deferred
tax (continued):
	 
	 	 	 	A deferred tax asset is recognized for unused tax losses and deductible temporary
differences, to the extent that it is probable that future taxable profits will be
available against which they can be utilized. Deferred tax assets are reviewed at each
reporting date and are reduced to the extent that it is no longer probable that the related
tax benefit will be realized.
	 
	 	(p)	 	Share-based compensation:
	 
	 	 	 	The Company records share-based compensation related to employee stock options granted
using the fair value based method estimated using the Black-Scholes model. Under this
method, compensation cost is measured at fair value at the date of grant and expensed, as
employee benefits, over the period in which employees unconditionally become entitled to
the award. The amount recognized as an expense is adjusted to reflect the number of awards
for which the related service conditions are expected to be met, such that the amount
ultimately recognized as an expense is based on the number of awards that do meet the
related service and non-market performance conditions at the vesting date.
	 
	 	 	 	Share-based payment arrangements in which the Company receives goods or services as
consideration for its own equity instruments are accounted for as equity-settled
share-based payment transactions, regardless of how the equity instruments are obtained by
the Company.
	 
	 	 	 	As permitted by IFRS 1, the Company elected not to restate options that were granted before
November 7, 2002 and those granted after November 7, 2002 that were fully vested prior to
the date of transition to IFRS.
	 
	 	(q)	 	Government grants:
	 
	 	 	 	Government grants consisting of grants and investment tax credits, are recorded as a
reduction of the related expense or cost of the asset acquired. Government grants are
recognized when there is reasonable assurance that the Company has met the requirements of
the approved grant program and there is reasonable assurance that the grant will be
received.

16

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(r)	 	Share capital:
	 
	 	 	 	Common shares:
	 
	 	 	 	Common shares are classified as equity. Incremental costs directly attributable to the
issue of common shares and share options are recognized as a deduction from equity, net of
any tax effects.
	 
	 	(s)	 	Earnings per share:
	 
	 	 	 	The Company presents basic and diluted earnings per share (“EPS”) data for its common shares. Basic EPS is calculated by dividing the net profit or loss attributable to common
shareholders of the Company by the weighted average number of common shares outstanding
during the period, adjusted for own shares held, if applicable. Diluted EPS is determined
by adjusting the profit or loss attributable to common shareholders and the weighted
average number of common shares outstanding, adjusted for own shares held if applicable,
for the effects of all dilutive potential common shares, which consist of the stock options
granted to employees.
	 
	 	(t)	 	New standards and interpretations not yet applied:
	 
	 	 	 	Certain pronouncements were issued by the IASB or International Financial Reporting
Interpretation Committee that are mandatory for annual periods beginning on or after
January 1, 2010 or later periods. Many of these updates are not applicable or are
inconsequential to the Company and have been excluded from the discussion below. The
remaining pronouncements are being assessed to determine their impact on the Company’s
results and financial position:
	 
	 	 	 	Annual improvements to IFRS:
	 
	 	 	 	The IASB’s improvements to IFRS published in April 2009 contain fifteen amendments to
twelve standards that result in accounting changes for presentation, recognition or
measurement purposes largely for annual periods beginning on or after January 1, 2010, with
early adoption permitted. These amendments were considered by the Company and deemed to be
not applicable to the Company other than for the amendment to IAS 17 — Leases relating to
leases which include both land and buildings elements. In this case, the Company early
adopted this amendment.
	 
	 	 	 	The IASB’s improvements to IFRS contain seven amendments that result in accounting changes
for presentation, recognition or measurement purposes. The most significant features of the
IASB’s annual improvements project published in May 2010 are included under the specific
revisions to standards discussed below.

17

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(t)	 	New standards and interpretations not yet applied (continued):
	 
	 	 	 	Annual improvements to IFRS (continued):

	 	(i)	 	IFRS 3:
	 
	 	 	 	Revision to IFRS 3, Business Combinations:
	 
	 	 	 	Effective for annual periods beginning on or after July 1, 2010 with earlier adoption
permitted.
	 
	 	 	 	Clarification on the following areas:

	 	•	 	the choice of measuring non-controlling interests at fair value or at the
proportionate share of the acquiree’s net assets applies only to instruments that
represent present ownership interests and entitle their holders to a proportionate
share of the net assets in the event of liquidation. All other components of
non-controlling interest are measured at fair value unless another measurement
basis is required by IFRS.
	 
	 	•	 	application guidance relating to the accounting for share-based payments
in IFRS 3 applies to all share-based payment transactions that are part of a
business combination, including unreplaced awards (i.e., unexpired awards over the
acquiree shares that remain outstanding rather than being replaced by the
acquirer) and voluntarily replaced share-based payment awards.

	 	(ii)	 	IFRS 7:
	 
	 	 	 	Amendment to IFRS 7, Financial Instruments: Disclosures:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2011, with earlier
adoption permitted.
	 
	 	 	 	Multiple clarifications related to the disclosure of financial instruments and in
particular in regards to transfers of financial assets.
	 
	 	(iii)	 	IAS 1:
	 
	 	 	 	Amendment to IAS 1, Presentation of Financial Statements:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2011, with earlier
adoption permitted.
	 
	 	 	 	Entities may present the analysis of the components of other comprehensive income
either in the statement of changes in equity or within the notes to the financial
statements.

18

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(t)	 	New standards and interpretations not yet applied (continued):
	 
	 	 	 	Annual improvements to IFRS (continued):

	 	(iv)	 	IAS 27:
	 
	 	 	 	Amendment to IAS 27, Consolidated and Separate Financial Statements:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2011, with earlier
adoption permitted.
	 
	 	 	 	The 2008 revisions to this standard resulted in consequential amendments to IAS 21,
The Effects of Changes in Foreign Exchange
Rates, IAS 28, Investments in Associates, and
IAS 31, Interests in Joint Ventures. IAS 27 now provides that these amendments are to be
applied prospectively.
	 
	 	(v)	 	IAS 34:
	 
	 	 	 	Amendment to IAS 34, Interim Financial Reporting:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2011, with earlier
adoption permitted.
	 
	 	 	 	The amendments place greater emphasis on the disclosure principles for interim financial
reporting involving significant events and transactions, including changes to fair value
measurements and the need to update relevant information from the most recent annual
report.

	 	 	 	New or revised standards and interpretations:
	 
	 	 	 	In addition, the following new or revised standards and interpretations have been issued but
are not yet applicable to the Company:

	 	(i)	 	IAS 24:
	 
	 	 	 	Amendments to IAS 24, Related Party Disclosures:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2011, with earlier
adoption permitted.
	 
	 	 	 	There are limited differences in the definition of what constitutes a related party;
however, the amendment requires more detailed disclosures regarding commitments.

19

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	3.	 	Significant accounting policies (continued):

	 	(t)	 	New standards and interpretations not yet applied (continued):
	 
	 	 	 	New or revised standards and interpretations (continued):

	 	(ii)	 	IFRS 8:
	 
	 	 	 	IFRS 8, Operating Segments:
	 
	 	 	 	Effective for annual periods beginning on or after January 1,
2010. Requires purchase information about segment assets.
	 
	 	(iii)	 	IFRS 9:
	 
	 	 	 	New standard IFRS 9, Financial Instruments:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2013, with earlier
adoption permitted.
	 
	 	 	 	As part of the project to replace IAS 39, Financial Instruments: Recognition and
Measurement, this standard retains but simplifies the mixed measurement model and
establishes two primary measurement categories for financial assets. More specifically,
the standard:

	 	•	 	deals with classification and measurement of financial assets
	 
	 	•	 	establishes two primary measurement categories for financial assets:
amortized cost and fair value
	 
	 	•	 	classification depends on entity’s business model and the contractual
cash flow characteristics of the financial asset
	 
	 	•	 	eliminates the existing categories: held to maturity, available for sale,
and loans and receivables.

	 	 	 	Certain changes were also made regarding the fair value option for financial
liabilities and accounting for certain derivatives linked to unquoted equity
instruments.

	4.	 	Revenue and deferred revenue:
	 
	 	 	On October 28, 2008, the Company entered into a collaboration and licensing agreement with EMD
Serono Inc. (“EMD Serono”), an affiliate of the Group Merck KGaA, of Darmstadt, Germany,
regarding the exclusive commercialization rights of tesamorelin in the United States for the
treatment of excess abdominal fat in HIV-infected patients with lipodystrophy (the “Initial
Product”). The Company retains all tesamorelin commercialization rights outside of the United
States.

20

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	4.	 	Revenue and deferred revenue (continued):
	 
	 	 	Under the terms of the agreement, the Company is responsible for the development of the Initial
Product up to obtaining marketing approval in the United States, which was obtained on November
10, 2010. The Company is also responsible for product production and for developing a new
formulation of the Initial Product. EMD Serono is responsible for conducting product
commercialization activities.
	 
	 	 	At the closing of the agreement on December 15, 2008, the Company received US$30,000
(C$36,951), which includes an initial payment of US$22,000 (C$27,097) and US$8,000 (C$9,854) as
a subscription for common shares in the Company by Merck KGaA at a price of US$3.67 (C$4.52)
per share. The Company may receive up to US$215,000, which amount includes the initial payment
of US$22,000, the equity investment of US$8,000, as well as payments based on the achievement
of certain development, regulatory and sales milestones. The Company will also be entitled to
receive increasing royalties on annual net sales of tesamorelin in the United States, if
applicable.
	 
	 	 	The initial payment of $27,097 has been deferred and is being amortized on a straight-line
basis over the estimated period for developing a new formulation of the Initial Product. This
period may be modified in the future based on additional information that may be received by
the Company. At November 30, 2010, an amount of $6,846 (2009 — $6,560) was recognized as
revenue. As at November 30, 2010, the deferred revenue related to this transaction amounted to
$13,692 (2009 — $20,537).
	 
	 	 	On August 12, 2009, the FDA accepted the New Drug Application (''NDA’’) made by the Company for
tesamorelin. Under the terms of the Company’s collaboration and licensing agreement with EMD
Serono, the acceptance of the tesamorelin NDA resulted in a milestone payment of US$10,000
(C$10,884).
	 
	 	 	On November 10, 2010, the FDA approved EGRIFTATM as the first approved
treatment in the United States for the reduction of excess abdominal fat in HIV-infected
patients with lipodystrophy. By virtue of the collaboration and licensing agreement entered
into in 2008 with EMD Serono, the Company received a milestone payment of US$25,000 (C$25,000)
associated with the FDA-approval of EGRIFTATM. This payment was received
by the Company on November 30, 2010.
	 
	 	 	The Company may conduct research and development activities for additional indications. Under
the collaboration and licensing agreement, EMD Serono will also have the option to
commercialize additional indications for tesamorelin in the United States. If it exercises this
option, EMD Serono will pay half of the development costs related to such additional
indications. In such cases, the Company will also have the right, subject to an agreement with
EMD Serono, to participate in promoting these additional indications.

21

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	5.	 	Personnel expenses:

	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	November 30,	 	 	November 30,	 
	 	 	Note	 	 	2010	 	 	2009	 
	 
	 	 	 	 	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Salaries and short-term employee benefits
	 	 	 	 	 	 	11,577	 	 	 	10,779	 
	Post-employment benefits
	 	 	 	 	 	 	579	 	 	 	542	 
	Termination benefits
	 	 	 	 	 	 	20	 	 	 	275	 
	Share-based compensation
	 	15 (iv)	 	 	1,133	 	 	 	997	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	 
	Total personnel expenses
	 	 	 	 	 	 	13,309	 	 	 	12,593	 
	 

	6.	 	Selling and market development expenses:
	 
	 	 	In 2008, the Company completed a formal review of the strategic alternatives regarding its
operations which culminated in the signing of the collaborative licensing agreement with EMD
Serono (note 4). As a result of this process, $4,269 was recorded in 2009 for professional fees
related to the closing of the agreement with EMD Serono.

	7.	 	Finance income and finance costs:
	 
	 	 	Recognized in net profit (loss):

	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 
	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 
	Interest income
	 	 	1,562	 	 	 	2,123	 
	Net gain on disposal of available-for-sale financial assets transferred from equity
	 	 	326	 	 	 	129	 
	 
	Finance income
	 	 	1,888	 	 	 	2,252	 
	 
	 	 	 	 	 	 	 	 
	Bank charges
	 	 	(18	)	 	 	(26	)
	Net foreign currency gain (loss)
	 	 	511	 	 	 	(635	)
	 
	Finance costs
	 	 	493	 	 	 	(661	)
	 
	 	 	 	 	 	 	 	 
	 
	Net finance income recognized in net profit (loss)
	 	 	2,381	 	 	 	1,591	 
	 

22

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	7.	 	Finance income and finance costs (continued):
	 
	 	 	Recognized in other comprehensive income:

	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 
	 	 	$	 	 	$	 
	 
	Net change in fair value of available-for-sale financial assets
	 	 	(390	)	 	 	1,039	 
	Net change in fair value of available-for-sale financial assets transferred to net profit (loss)
	 	 	(326	)	 	 	(129	)
	 
	 
	Finance (costs) income recognized in other comprehensive income, net of tax
	 	 	(716	)	 	 	910	 
	 

	8.	 	Bonds:
	 
	 	 	Bonds are interest-bearing available-for-sale financial assets, with a carrying amount of
$37,901 as at November 30, 2010 ($61,843 in 2009, and $46,204 as at December 1, 2008), have
stated interest rates of 2.37% to 6.75% (2.37% to 6.75% in 2009 and 3.00% to 6.85% as at
December 1, 2008) and mature in 1.9 year (2.16 in 2009 and 1.8 in 2008).
	 
	 	 	The Company’s exposure to credit and interest rate risks related to bonds is presented in note
20.

	9.	 	Trade and other receivables:

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	November 30,	 	 	November 30,	 	 	December 1,	 
	 	 	Note	 	 	2010	 	 	2009	 	 	2008	 
	 
	 	 	 
	 	 	$	 	 	$	 	 	$	 
	 
	Trade receivables
	 	 	 	 	 	 	6	 	 	 	3	 	 	 	12	 
	Sales tax receivable
	 	 	 	 	 	 	100	 	 	 	190	 	 	 	419	 
	Loans granted to employees under the share purchase plan
	 	15 (iii)	 	 	25	 	 	 	74	 	 	 	91	 
	Loans granted to related parties under the share purchase plan
	 	15 (iii)	 	 	22	 	 	 	75	 	 	 	59	 
	Other receivables
	 	 	 	 	 	 	8	 	 	 	33	 	 	 	29	 
	 
	 
	 
	 	 	 	 	 	 	161	 	 	 	375	 	 	 	610	 
	 

	 	 	The Company’s exposure to credit and currency risks related to trade and other receivables
is presented in note 20.

23

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	10.	 	Tax credits and grants receivable:

	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 
	 	 	$	 	 	$	 
	 
	Balance at beginning of the year
	 	 	1,333	 	 	 	1,451	 
	Investment tax credits and grants received
	 	 	(1,935	)	 	 	(1,913	)
	Investment tax credits and grants recognized in net profit (loss)
	 	 	934	 	 	 	1,795	 
	 
	 
	 
	 	 	332	 	 	 	1,333	 
	 

Tax credits and grants receivable comprise research and development investment tax credits
receivable from the provincial government which relate to qualifiable research and development
expenditures under the applicable tax laws. The amounts recorded as receivable are subject to a
government tax audit and the final amounts received may differ from those recorded. There are
no unfulfilled conditions or contingencies associated with the government assistance received.

Unused federal tax credits may be used to reduce future income tax and expire as follows:

	 	 	 	 	 
	 	 	$	 
	 
	 
	2023
	 	 	452	 
	2024
	 	 	1,597	 
	2025
	 	 	1,863	 
	2026
	 	 	2,178	 
	2027
	 	 	3,000	 
	2028
	 	 	3,328	 
	2029
	 	 	2,250	 
	2030
	 	 	1,167	 
	 
	 
	 
	 	 	15,835	 
	 

	11.	 	Inventories:

	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 	 	December 1,	 
	 	 	2010	 	 	2009	 	 	2008	 
	 
	 	 	$	 	 	$	 	 	$	 
	 
	Raw materials
	 	 	3,395	 	 	 	2,225	 	 	 	—	 
	Work in progress
	 	 	922	 	 	 	—	 	 	 	—	 
	 
	 
	 
	 	 	4,317	 	 	 	2,225	 	 	 	—	 
	 

24

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	11.	 	Inventories (continued):
	 
	 	 	In 2010, $123 of raw materials, and $69 of work in progress were written down to their net
realizable value (November 30, 2009 — nil and nil; December 1, 2008 — nil and nil).
Consequently, a write-down of $192 was recorded to cost of sales in 2010 (2009 — nil).
	 
	 	 	The write-down was due to unfavourable pricing related to raw materials that were not
originally purchased under the conditions of the Company’s current long-term procurement
agreements.
	 
	12.	 	Property and equipment:

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	Office	 	 	 	 	 	 	 
	 	 	Computer	 	 	Laboratory	 	 	furniture and	 	 	Leasehold	 	 	 	 
	 	 	equipment	 	 	equipment	 	 	equipment	 	 	improvements	 	 	Total	 
	 	 	$	 	 	$	 	 	$	 	 	$	 	 	$	 
	 
	Cost:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Balance at December 1, 2008
	 	 	682	 	 	 	1,824	 	 	 	1,015	 	 	 	1,846	 	 	 	5,367	 
	Additions
	 	 	222	 	 	 	125	 	 	 	188	 	 	 	8	 	 	 	543	 
	Disposals
	 	 	(30	)	 	 	(4	)	 	 	(79	)	 	 	—	 	 	 	(113	)
	 
	Balance at November 30, 2009
	 	 	874	 	 	 	1,945	 	 	 	1,124	 	 	 	1,854	 	 	 	5,797	 
	 
	Additions
	 	 	130	 	 	 	116	 	 	 	7	 	 	 	46	 	 	 	299	 
	Disposals
	 	 	(63	)	 	 	(43	)	 	 	(2	)	 	 	—	 	 	 	(108	)
	 
	Balance at November 30, 2010
	 	 	941	 	 	 	2,018	 	 	 	1,129	 	 	 	1,900	 	 	 	5,988	 
	 
	Accumulated depreciation:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Balance at December 1, 2008
	 	 	500	 	 	 	1,427	 	 	 	700	 	 	 	1,441	 	 	 	4,068	 
	 
	Depreciation for the year
	 	 	147	 	 	 	96	 	 	 	79	 	 	 	290	 	 	 	612	 
	Disposals
	 	 	(30	)	 	 	(4	)	 	 	(78	)	 	 	—	 	 	 	(112	)
	 
	Balance at November 30, 2009
	 	 	617	 	 	 	1,519	 	 	 	701	 	 	 	1,731	 	 	 	4,568	 
	Depreciation for the year
	 	 	170	 	 	 	88	 	 	 	85	 	 	 	123	 	 	 	466	 
	Disposals
	 	 	(63	)	 	 	(41	)	 	 	(2	)	 	 	—	 	 	 	(106	)
	 
	Balance at November 30, 2010
	 	 	724	 	 	 	1,566	 	 	 	784	 	 	 	1,854	 	 	 	4,928	 
	 
	 
	Net carrying amounts:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	December 1, 2008
	 	 	182	 	 	 	397	 	 	 	315	 	 	 	405	 	 	 	1,299	 
	November 30, 2009
	 	 	257	 	 	 	426	 	 	 	423	 	 	 	123	 	 	 	1,229	 
	November 30, 2010
	 	 	217	 	 	 	452	 	 	 	345	 	 	 	46	 	 	 	1,060	 
	 
	 

25

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	12.	 	Property and equipment (continued):
	 
	 	 	Depreciation expense for the year has been recorded in the following accounts in the
consolidated statement of comprehensive income:

	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 
	 	 	$	 	 	$	 
	Cost of sales
	 	 	8	 	 	 	—	 
	Research and development expenses
	 	 	231	 	 	 	306	 
	Selling and market development expenses
	 	 	10	 	 	 	14	 
	General and administrative expenses
	 	 	217	 	 	 	292	 
	 
	 
	 	 	466	 	 	 	612	 
	 

	13.	 	Accounts payable and accrued liabilities:

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	November 30,	 	 	November 30,	 	 	December 1,	 
	 	 	 	Note	 	 	2010	 	 	2009	 	 	2008	 
	 
	 	 	 	 	 	 	$	 	 	$	 	 	$	 
	Trade payables
	 	 	 	 	 	 	1,001	 	 	 	1,984	 	 	 	284	 
	Accrued liabilities and other payables
	 	 	 	 	 	 	1,440	 	 	 	1,768	 	 	 	4,692	 
	Salaries and benefits due to related parties
	 	 	25	 	 	 	565	 	 	 	450	 	 	 	504	 
	Employee salaries and benefits payable
	 	 	 	 	 	 	1,971	 	 	 	1,366	 	 	 	1,385	 
	 
	 
	 	 	 	 	 	 	4,977	 	 	 	5,568	 	 	 	6,865	 
	 

The Company’s exposure to currency and liquidity risks related to accounts payable and
accrued liabilities is presented in note 20.

	14.	 	Other liabilities:
	 
	 	 	Other liabilities consist of deferred lease inducements relating to rent free periods amounting
to $325 as at November 30, 2010 (November 30, 2009 and December 1, 2008 — nil) (note 17).

26

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	15.	 	Share capital:
	 
	 	 	Authorized in unlimited number and without par value:

	 	 	 	Common shares
	 
	 	 	 	Preferred shares issuable in one or more series

All issued shares are fully paid, except for 33,524 (2009 — 90,298) issued under the share
purchase plan and for which the loan has not been repaid in full (see note 15 (iii)).

Common shareholders are entitled to receive dividends as declared by the Company at its
discretion and are entitled to one vote per share at the Company’s annual general meeting.

No preferred shares are outstanding.

	 	(i)	 	2010:
	 
	 	 	 	In 2010, the Company received subscriptions in the amount of $15 for the issuance of 2,880
common shares in connection with its share purchase plan.
	 
	 	 	 	2009:
	 
	 	 	 	Under the terms of the collaboration and licensing agreement with EMD Serono, the Company
issued 2,179,837 common shares for a cash consideration of $9,854 (see note 4).
	 
	 	 	 	In 2009, the Company also received subscriptions in the amount of $96 for the issuance of
34,466 common shares in connection with its share purchase plan.
	 
	 	 	 	All shares issued were for cash consideration.
	 
	 	(ii)	 	Shareholder rights plan:
	 
	 	 	 	On February 10, 2010, the Company’s Board of Directors adopted a shareholder rights plan
(the ''Plan’’), effective as of that date. The Plan is designed to provide adequate time
for the Board of Directors and the shareholders, to assess an unsolicited takeover bid for
the Company. In addition, the Plan provides the Board of Directors with sufficient time to
explore and develop alternatives for maximizing shareholder value if a takeover bid is
made, as well as provide shareholders with an equal opportunity to participate in a
takeover bid to receive full and fair value for their common shares. The Plan will expire
at the close of the Company’s annual meeting of shareholders in 2013.

27

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	15.	 	Share capital (continued):

	 	(ii)	 	Shareholder rights plan (continued):
	 
	 	 	 	The rights issued under the Plan will initially attach to and trade with the common shares
and no separate certificates will be issued unless a triggering event occurs. The rights
will become exercisable only when a person, including any party related to it, acquires or
attempts to acquire 20% or more of the outstanding shares without complying with the
“Permitted Bid” provisions of the Plan or without approval of the Board of Directors.
Should such an acquisition occur or be announced, each right would, upon exercise, entitle
a rights holder, other than the acquiring person and related persons, to purchase common shares at a 50% discount to the market price at the time.
	 
	 	 	 	Under the Plan, a Permitted Bid is a bid made to all holders of the common shares and which
is open for acceptance for not less than 60 days. If at the end of 60 days at least 50% of
the outstanding common shares, other than those owned by the offeror and certain related
parties, have been tendered, the offeror may take up and pay for the common shares, but
must extend the bid for a further 10 days to allow other shareholders to tender.
	 
	 	(iii)	 	Share purchase plan:
	 
	 	 	 	The Share Purchase Plan entitles full-time and part-time employees of the Company who, on
the participation date, are residents of Canada, are not under a probationary period and do
not hold, directly or indirectly, five percent (5%) or more of the Company’s outstanding
common shares, to directly subscribe for common shares of the Company. Under the Share
Purchase Plan, a maximum of 550,000 common shares may be issued to employees.
	 
	 	 	 	On May 1 and November 1 of each year (the “Participation Dates”), an employee may
subscribe for a number of common shares under the Share Purchase Plan for an amount that
does not exceed 10% of that employee’s gross annual salary for that year. Under the Share
Purchase Plan, the Board of Directors has the authority to suspend or defer a subscription
of common shares, or to decide that no subscription of common shares will be allowed on a
Participation Date if it is in the Company’s best interest.
	 
	 	 	 	The Share Purchase Plan provides that the number of common shares that may be issued to
insiders, at any time, under all share-based compensation arrangements of the Company,
cannot exceed 10% of the Company’s outstanding common shares, and the number of common shares issued to insiders, within any one-year period, under all security-based
compensation arrangements, cannot exceed 10% of the outstanding common shares.
	 
	 	 	 	The subscription price for each new common share subscribed for under the Share Purchase
Plan is equal to the weighted average closing price of the common shares on the Toronto
Stock Exchange during a period of five days prior to the Participation Date. Employees may
not assign the rights granted under the Share Purchase Plan.

28

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	15.	 	Share capital (continued):

	 	(iii)	 	Share purchase plan (continued):
	 
	 	 	 	An employee may elect to pay the subscription price for common shares in cash or through an
interest-free loan from the Company. Loans granted by the Company under the Share Purchase
Plan are repayable through salary withholdings over a period not exceeding two years. All
loans may be repaid prior to the scheduled repayment at any time. The loans granted to any
employee may at no time exceed 10% of that employee’s current annual gross salary. All
common shares purchased through an interest-free loan are hypothecated to secure full and
final repayment of the loan and are held by a trustee until repayment in full. Loans are
immediately due and payable on the occurrence of any of the following events:
(i) termination of employment; (ii) sale or seizure of the hypothecated common shares;
(iii) bankruptcy or insolvency of the employee; or (iv) suspension of the payment of
an employee’s salary or revocation of the employee’s right to salary withholdings.
	 
	 	 	 	At November 30, 2010, $47 (November 30, 2009 — $149; December 1, 2008 — $150) was
receivable under these loans (see note 9).
	 
	 	(iv)	 	Stock option plan:
	 
	 	 	 	The Company has established a stock option plan under which it can grant to its directors,
officers, employees, researchers and consultants non-transferable options for the purchase
of common shares. The exercise date of an option may not be later than 10 years after the
grant date. A maximum number of 5,000,000 options can be granted under the plan. Generally,
the options vest at the date of the grant or over a period up to 5 years. As at November
30, 2010, 981,005 options could still be granted by the Company (2009 — 1,244,834).
	 
	 	 	 	All options are to be settled by physical delivery of shares.

29

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	15.	 	Share capital (continued):

	 	(iv)	 	Stock option plan (continued):
	 
	 	 	 	Changes in the number of options outstanding during the past two years were as follows:

	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	Weighted	 
	 	 	 	 	 	 	average	 
	 	 	 	 	 	 	exercise price	 
	 	 	Options	 	 	per option	 
	 	 	 	 	 	 	$	 
	 
	 	 	 	 	 	 	 	 
	Options at December 1, 2008
	 	 	2,161,800	 	 	 	6.52	 
	 
	 	 	 	 	 	 	 	 
	Granted
	 	 	680,500	 	 	 	1.83	 
	Expired
	 	 	(58,500	)	 	 	5.16	 
	Forfeited
	 	 	(118,000	)	 	 	9.92	 
	 
	 	 	 	 	 	 	 	 
	 
	Options at November 30, 2009
	 	 	2,665,800	 	 	 	5.20	 
	 
	 	 	 	 	 	 	 	 
	Granted
	 	 	335,000	 	 	 	4.03	 
	Expired
	 	 	(32,500	)	 	 	11.15	 
	Forfeited
	 	 	(38,671	)	 	 	3.61	 
	Exercised (weighted average share price: $5.14)
	 	 	(80,491	)	 	 	1.66	 
	 
	 	 	 	 	 	 	 	 
	 
	Options at November 30, 2010
	 	 	2,849,138	 	 	 	5.12	 
	 
	Exercisable at November 30, 2010
	 	 	2,196,403	 	 	 	5.77	 
	 

	 
	 	 	 	The following table provides stock option information as at November 30, 2010:     

	 	 	 	 	 	 	 	 	 	 	 	 	 
	Options outstanding	 
	 	 	 	 	 	 	Weighted	 	 	 	 
	 	 	 	 	 	 	average	 	 	Weighted	 
	 	 	Number of	 	 	remaining	 	 	average	 
	 	 	options	 	 	life	 	 	exercise	 
	Price range ($)	 	outstanding	 	 	(years)	 	 	price	 
	 	 	 	 	 	 	 	 	 	 	$	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	1.20 — 2.00
	 	 	1,183,015	 	 	 	6.54	 	 	 	1.71	 
	2.01 — 2.75
	 	 	141,459	 	 	 	3.85	 	 	 	2.59	 
	2.76 — 3.75
	 	 	70,000	 	 	 	5.51	 	 	 	3.37	 
	3.76 — 4.60
	 	 	265,000	 	 	 	9.03	 	 	 	3.84	 
	4.61 — 6.00
	 	 	95,000	 	 	 	7.69	 	 	 	4.93	 
	6.01 — 9.00
	 	 	570,664	 	 	 	4.82	 	 	 	8.17	 
	9.01 — 13.50
	 	 	480,000	 	 	 	2.86	 	 	 	10.72	 
	13.51 — 15.30
	 	 	44,000	 	 	 	0.36	 	 	 	15.12	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	 
	 
	 	 	2,849,138	 	 	 	5.59	 	 	 	5.12	 
	 

30

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	15.	 	Share capital (continued):

	 	(iv)	 	Stock option plan (continued):
	 
	 	 	 	The fair value of options granted was estimated at the grant date using the Black-Scholes
model and the following weighted average assumptions:

	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 
	 
	 	 	 	 	 	 	 	 
	Risk-free interest rate
	 	 	2.49	%	 	 	1.83	%
	Expected volatility
	 	 	81.13	%	 	 	79.50	%
	Average option life in years
	 	 	7.5	 	 	 	7.5	 
	Expected dividends
	 	 	nil	 	 	 	nil	 
	Grant-date share price
	 	$	4.03	 	 	$	1.83	 
	Option exercise price
	 	$	4.03	 	 	$	1.83	 

	 	 	 	The risk-free interest rate is based on the implied yield on a Canadian Government
zero-coupon issue with a remaining term equal to the expected term of the option. The
volatility is based solely on historical volatility equal to the expected life of the
option. The life of the options is estimated considering the vesting period at the grant
date, the life of the option and the average length of time similar grants have remained
outstanding in the past. The dividend yield was excluded from the calculation since it is
the present policy of the Company to retain all earnings to finance operations and future
growth.
	 
	 	 	 	The following table summarizes the measurement date weighted average fair value of stock
options granted during the years ended November 2010 and 2009:

	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	Weighted	 
	 	 	 	 	 	 	average	 
	 	 	Number of	 	 	grant-date	 
	 	 	options	 	 	fair value	 
	 	 	 	 	 	 	$	 
	 
	 	 	 	 	 	 	 	 
	2010
	 	 	335,000	 	 	 	3.05	 
	2009
	 	 	680,500	 	 	 	1.36	 

	 	 	 	The Black-Scholes model used by the Company to calculate option values was developed
to estimate the fair value of freely tradable, fully transferable options without vesting
restrictions, which significantly differs from the Company’s stock option awards. This
model also requires four highly subjective assumptions, including future stock price
volatility and average option life, which greatly affect the calculated values.

31

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	15.	 	Share capital (continued):

	 	(v)	 	Earnings per share:
	 
	 	 	 	The calculation of basic earnings per share at November 30, 2010 was based on the net
profit (loss) attributable to common shareholders of the Company of $8,930 (2009 -
($15,156)), and a weighted average number of common shares outstanding of 60,480,032 (2009
 — 60,314,309), calculated as follows:

	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 
	 
	 	 	 	 	 	 	 	 
	Issued common shares at December 1
	 	 	60,429,393	 	 	 	58,215,090	 
	Effect of share options exercised
	 	 	49,030	 	 	 	—	 
	Effect of shares issued during the year
	 	 	1,609	 	 	 	2,099,219	 
	 
	 	 	 	 	 	 	 	 
	 
	Weighted average number of common shares at November 30
	 	 	60,480,032	 	 	 	60,314,309	 
	 

	 	 	 	The calculation of diluted earnings per share was based on a weighted average number
of common shares calculated as follows:

	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 
	 
	 	 	 	 	 	 	 	 
	Weighted average number of common shares (basic)
	 	 	60,480,032	 	 	 	60,314,309	 
	Effect of stock options on issue
	 	 	842,959	 	 	 	—	 
	 
	 	 	 	 	 	 	 	 
	 
	Weighted average number of common shares (diluted) at November 30
	 	 	61,322,991	 	 	 	60,314,309	 
	 

	 	 	 	At November 30, 2010, 1,119,664 options (2009 — 1,371,167) were excluded from the
diluted weighted average number of common shares calculation as their effect would have
been anti-dilutive.
	 
	 	 	 	The average market value of the Company’s shares for purposes of calculating the dilutive
effect of share options was based on quoted market prices for the period during which the
options were outstanding.

32

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	16.	 	Income taxes:
	 
	 	 	Current tax expense:

	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 
	Current tax expense:
	 	 	 	 	 	 	 	 
	Current tax expense for the year
	 	 	3,285	 	 	 	—	 
	Recognition of previously unrecognized tax losses
	 	 	(3,171	)	 	 	—	 
	 
	 	 	 	 	 	 	 	 
	 
	Current Income tax expense
	 	 	114	 	 	 	—	 
	 
	 
	 	 	 	 	 	 	 	 
	Deferred tax expense:
	 	 	 	 	 	 	 	 
	Recognition and reversal of temporary differences
	 	 	—	 	 	 	(4,031	)
	Change in unrecognized deductible temporary differences
	 	 	—	 	 	 	4,031	 
	 
	 	 	 	 	 	 	 	 
	 
	Deferred income tax expense
	 	 	—	 	 	 	—	 
	 
	 
	 	 	 	 	 	 	 	 
	Total income tax expense
	 	 	114	 	 	 	—	 
	 

	 
	 
	 
	 
	 
	 	 	Reconciliation between effective and applicable tax amounts:     

	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 
	Income taxes at domestic tax statutory rate
	 	 	2,713	 	 	 	(4,683	)
	Change in unrecognized deductible temporary differences
	 	 	(3,171	)	 	 	4,031	 
	Non-deductible expenses and other
	 	 	572	 	 	 	652	 
	 
	 	 	 	 	 	 	 	 
	 
	 
	 	 	114	 	 	 	—	 
	 

	 	 	Deferred tax assets:
	 
	 	 	Deferred tax asset of $114 (2009 — nil) related to share issue costs was recognized directly in
equity.

33

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	16.	 	Income taxes (continued):
	 
	 	 	Deferred tax assets (continued):
	 
	 	 	Unrecognized deferred tax assets:
	 
	 	 	At November 30, 2010, temporary differences for which no deferred tax asset was recognized were
as follows:

	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 
	Long-term:
	 	 	 	 	 	 	 	 
	Research and development expenses
	 	 	30,143	 	 	 	29,380	 
	Deferred non-capital losses
	 	 	21,013	 	 	 	21,490	 
	Property and equipment
	 	 	609	 	 	 	674	 
	Intellectual property and patent fees
	 	 	9,230	 	 	 	12,307	 
	Available deductions and other
	 	 	4,648	 	 	 	4,963	 
	 
	 	 	 	 	 	 	 	 
	 
	 
	 	 	65,643	 	 	 	68,814	 
	 

	 	 	In assessing the realizability of deferred tax assets, management considers whether it is
more likely than not that some portion or all of the deferred tax assets will not be realized.
The ultimate realization of deferred tax assets is dependent upon the generation of future
taxable income. The generation of future taxable income is dependent on the successful
commercialization of the Company’s products and technologies.
	 
	 	 	Given the Company’s past losses, management does not believe that it is more probable than not
that the Company can realize its deferred tax assets and therefore it has not recognized any
amount in the statement of financial position.

34

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	16.	 	Income taxes (continued):
	 
	 	 	Deferred tax assets (continued):
	 
	 	 	Unrecognized deferred tax assets (continued):
	 
	 	 	At November 30, 2010, the amounts and expiry dates of tax attributes to be deferred for which
no deferred tax asset was recognized were as follows:

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	November 30,	 	 	 	 	 	 	November 30,	 
	 	 	 	 	 	 	2010	 	 	 	 	 	 	2009	 
	 
	 	 	Federal	 	 	Provincial	 	 	Federal	 	 	Provincial	 
	 
	 	 	$	 	 	$	 	 	$	 	 	$	 
	Research and development expenses,
without time limitation
	 	 	103,324	 	 	 	123,062	 	 	 	103,346	 	 	 	115,686	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Losses carried forward:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	2014
	 	 	1,216	 	 	 	—	 	 	 	9,603	 	 	 	—	 
	2015
	 	 	275	 	 	 	—	 	 	 	275	 	 	 	—	 
	2027
	 	 	7,638	 	 	 	7,628	 	 	 	7,638	 	 	 	7,628	 
	2028
	 	 	46,316	 	 	 	32,174	 	 	 	46,316	 	 	 	46,271	 
	2029
	 	 	19,484	 	 	 	16,467	 	 	 	21,785	 	 	 	18,802	 
	2030
	 	 	11,440	 	 	 	11,436	 	 	 	—	 	 	 	—	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Other temporary differences, without time limitation:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Excess of tax value of property and equipment
over carrying value
	 	 	2,773	 	 	 	1,666	 	 	 	3,121	 	 	 	1,785	 
	Tax value of intellectual property and patent fees
	 	 	34,301	 	 	 	34,289	 	 	 	45,735	 	 	 	45,718	 
	Available deductions and other
	 	 	57,343	 	 	 	1,412	 	 	 	58,415	 	 	 	2,732	 

	17.	 	Operating leases:
	 
	 	 	The Company rents its headquarters and main office pursuant to an operating lease (the
“Lease”) expiring in April 2021. Under the terms of the Lease, the Company has also been
granted two renewal options for periods of five years each. Lease payments will increase by 11%
beginning on November 1, 2015.
	 
	 	 	During the year ended November 30, 2010, an amount of $628 was recognized as an expense in
respect of operating leases (2009 — $805). Of the amount $133 (2009 — $176) is included in
General and administrative expenses and $495 (2009 — $629) is included in Research and
development expenses.

35

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	17.	 	Operating leases (continued):
	 
	 	 	The Company’s lease includes a lease of land and building. Since the land title does not pass,
and the Company does not participate in the residual value of the building, it was determined
that substantially all the risks and rewards of the building are with the lessor. As such, the
Company determined that the lease is an operating lease.
	 
	 	 	The Company has committed to pay the lessor for its share of some operating expenses of the
leased premises. This amount has been set at $240 per year beginning May 1, 2010 and will be
increased by 2.5% annually for the duration of the Lease. Refer to note 23 for the contractual
commitments related to this lease.
	 
	 	 	The lessor granted the Company a monetary allowance in the amount of $728 to make leasehold
improvements. This amount had not been received as at November 30, 2010. Furthermore, the
Company benefits from a 25-month rent free period which is deferred and recognized over the
lease term. As at November 30, 2010, $325 was included in Other liability (nil — November 30,
2009) in regards to the deferred free rent inducement (note 14 — Other liabilities).
	 
	 	 	The Company had issued an irrevocable letter of credit in favour of the lessor in the amount of
$323 under the terms of the Lease renewal, along with a first ranking movable hypothec in the
amount of $1,150 covering all the Company’s tangible assets located in the rented premises. The
letter of credit and the hypothec were cancelled on April 30, 2010.
	 
	18.	 	Contingent liability:
	 
	 	 	On July 26, 2010, the Company received a motion of authorization to institute a class action
lawsuit against the Company, a director and a former executive officer (the “Motion”). This
Motion was filed in the Superior Court of Quebec, district of Montreal. The applicant is
seeking to initiate a class action suit to represent the class of persons who were shareholders
at May 21, 2010 and who sold their common shares of the Company on May 25 or 26, 2010. This
applicant alleges that the Company did not comply with its continuous disclosure obligations as
a reporting issuer by failing to disclose certain alleged adverse effects relating to the
administration of EGRIFTATM. The Company is of the view that the
allegations contained in the Motion are entirely without merit and intends to take all
appropriate actions to vigorously defend its position.
	 
	 	 	The Motion had not yet been heard by the Superior Court of Quebec and a date has not been set
for the hearing.

36

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	18.	 	Contingent liability (continued):
	 
	 	 	The Company has subscribed to insurance covering its potential liability and the potential
liability of its directors and officers in the performance of their duties for the Company
subject to a $200 deductible. At November 30, 2010, an amount of $96 in legal fees has been
accrued and included in general and administrative expenses, of which $61 was paid during the
year and $35 remained in accounts payable and accrued liabilities.
	 
	19.	 	Statement of cash flows:
	 
	 	 	The Company entered into the following transactions which had no impact on the cash flows:

	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 	 	December 1,	 
	 	 	2010	 	 	2009	 	 	2008	 
	 
	 	 	$	 	 	$	 	 	$	 
	 
	Additions to property and equipment included in accounts
payable and accrued liabilities
	 	 	65	 	 	 	183	 	 	 	48	 
	Share issue costs included in accounts payable and accrued liabilities
	 	 	—	 	 	 	—	 	 	 	8	 

	 	 	In addition, interest received totalled $2,290 (2009 — $1,200).
	 
	20.	 	Financial instruments:
	 
	 	 	Overview:
	 
	 	 	This note provides disclosures relating to the nature and extent of the Company’s exposure to
risks arising from financial instruments, including credit risk, liquidity risk, currency risk
and interest rate risk, and how the Company manages those risks.

	 	(a)	 	Credit risk:
	 
	 	 	 	Credit risk is the risk of an unexpected loss if a customer or counterparty to a financial
instrument fails to meet its contractual obligations. The Company regularly monitors credit
risk exposure and takes steps to mitigate the likelihood of this exposure resulting in
losses.

37

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	20.	 	Financial instruments (continued):
	 
	 	 	Overview (continued):

	 	(a)	 	Credit risk (continued):
	 
	 	 	 	The Company’s exposure to credit risk currently relates to accounts receivable with only
one customer (see note 4). Financial instruments other than cash and trade and other
receivables that potentially subject the Company to significant credit risk consist
principally of bonds. The Company invests its available cash in highly liquid fixed income
instruments from governmental, paragovernmental and municipal bodies ($37,542 as at
November 30, 2010) as well as from companies with high credit ratings ($359 as at November
30, 2010). As at November 30, 2010, the Company was not exposed to any credit risk over the
carrying amount of the bonds.
	 
	 	(b)	 	Liquidity risk:
	 
	 	 	 	Liquidity risk is the risk that the Company will not be able to meet its financial
obligations as they become due. As indicated in the capital management section below, the
Company manages this risk through the management of its capital structure. It also manages
liquidity risk by continuously monitoring actual and projected cash flows. The Board of
Directors and/or the Audit Committee reviews and approves the Company’s operating and
capital budgets, as well as any material transactions out of the ordinary course of
business.
	 
	 	 	 	The Company has adopted an investment policy in respect of the safety and preservation of
its capital to ensure the Company’s liquidity needs are met. The instruments are selected
with regard to the expected timing of expenditures and prevailing interest rates.
	 
	 	 	 	The following are amounts due on the contractual maturities of financial liabilities as at
November 30, 2010 and 2009:

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	November 30,	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	2010	 
	 
	 	 	 	 	 	 	Carrying	 	 	Less than	 	 	1 to	 	 	More than	 
	 	 	Total	 	 	amount	 	 	1 year	 	 	5 years	 	 	5 years	 
	 
	 	 	$	 	 	$	 	 	$	 	 	$	 	 	$	 
	 
	Accounts payable and accrued liabilities
	 	 	4,977	 	 	 	4,977	 	 	 	4,977	 	 	 	—	 	 	 	—	 

38

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	20.	 	Financial instruments (continued):
	 
	 	 	Overview (continued):

	 	(b)	 	Liquidity risk (continued):

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	November 30,	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	2009	 
	 
	 	 	 	 	 	 	Carrying	 	 	Less than	 	 	1 to	 	 	More than	 
	 	 	Total	 	 	amount	 	 	1 year	 	 	5 years	 	 	5 years	 
	 
	 	 	$	 	 	$	 	 	$	 	 	$	 	 	$	 
	 
	Accounts payable and accrued liabilities
	 	 	5,568	 	 	 	5,568	 	 	 	5,568	 	 	 	—	 	 	 	—	 

	 	(c)	 	Currency risk:
	 
	 	 	 	The Company is exposed to financial risk related to the fluctuation of foreign exchange
rates and the degree of volatility of those rates. Currency risk is limited to the portion
of the Company’s business transactions denominated in currencies other than the Canadian
dollar, primarily revenues from milestone payments and expenses for research and
development incurred in US dollars, euros and pounds sterling (“GBP”). The Company does
not use derivative financial instruments to reduce its foreign exchange exposure.
	 
	 	 	 	The Company manages currency risk by maintaining cash in US dollars on hand to support US
forecasted cash budgets for a maximum 12-month period. The Company does not currently view
its exposure to the euro and GBP as a significant foreign exchange risk due to the limited
volume of transactions conducted by the Company in these currencies.
	 
	 	 	 	Exchange rate fluctuations for foreign currency transactions can cause cash flows as well
as amounts recorded in the consolidated statement of comprehensive income to vary from
period to period and not necessarily correspond to those forecasted in operating budgets
and projections. Additional earnings variability arises from the translation of monetary
assets and liabilities denominated in currencies other than the Canadian dollar at the
rates of exchange at each consolidated statement of financial position date, the impact of
which is reported as foreign exchange gain or loss in the consolidated statement of
comprehensive income. Given the Company’s policy on the management of the Company’s US
foreign currency risk, the Company does not believe a sudden change in foreign exchange
rates would impair or enhance its ability to pay its US dollar denominated obligations.

39

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	20.	 	Financial instruments (continued):
	 
	 	 	Overview (continued):

	 	(c)	 	Currency risk (continued):
	 
	 	 	 	The following table presents the significant items exposed to currency risk at the
following dates:

	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	November 30,	 
	 	 	 	 	 	 	 	 	 	 	2010	 
	 
	 	 	$US	 	 	EURO	 	 	GBP	 
	 
	 
	Cash
	 	 	26,424	 	 	 	—	 	 	 	1	 
	Trade and other receivables
	 	 	—	 	 	 	—	 	 	 	—	 
	Accounts payable and accrued liabilities
	 	 	(465	)	 	 	(26	)	 	 	(81	)
	 
	 
	Items exposed to currency risk
	 	 	25,959	 	 	 	(26	)	 	 	(80	)
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	November 30,	 
	 	 	 	 	 	 	 	 	 	 	2009	 
	 
	 	 	$US	 	 	EURO	 	 	GBP	 
	 
	 
	Cash
	 	 	1,471	 	 	 	—	 	 	 	—	 
	Trade and other receivables
	 	 	—	 	 	 	4	 	 	 	—	 
	Accounts payable and accrued liabilities
	 	 	(1,095	)	 	 	—	 	 	 	(25	)
	 
	 
	Items exposed to currency risk
	 	 	376	 	 	 	4	 	 	 	(25	)
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	December 1,	 
	 	 	 	 	 	 	 	 	 	 	2008	 
	 
	 	 	$US	 	 	EURO	 	 	GBP	 
	 
	 
	Cash
	 	 	1	 	 	 	—	 	 	 	—	 
	Trade and other receivables
	 	 	—	 	 	 	—	 	 	 	—	 
	Accounts payable and accrued liabilities
	 	 	(2,589	)	 	 	(159	)	 	 	(348	)
	 
	 
	Items exposed to currency risk
	 	 	(2,588	)	 	 	(159	)	 	 	(348	)
	 

40

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008 

(in thousands of Canadian dollars, except per share amounts)
 

	20.	 	Financial instruments (continued):
	 
	 	 	Overview (continued):

	 	(c)	 	Currency risk (continued):
	 
	 	 	 	The following exchange rates are those applicable to the following periods and dates:

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 	 	December 1,	 
	 	 	2010	 	 	2009	 	 	2008	 
	 
	 	 	Average	 	 	Reporting	 	 	Average	 	 	Reporting	 	 	Average	 	 	Reporting	 
	 	 	rate	 	 	date rate	 	 	rate	 	 	date rate	 	 	rate	 	 	date rate	 
	 
	$US — C$
	 	 	1.0345	 	 	 	1.0266	 	 	 	1.0594	 	 	 	1.0556	 	 	 	1.0479	 	 	 	1.2370	 
	EURO — C$
	 	 	1.3848	 	 	 	1.3326	 	 	 	1.5808	 	 	 	1.5852	 	 	 	1.5440	 	 	 	1.5711	 
	GBP — C$
	 	 	1.6051	 	 	 	1.5969	 	 	 	1.7597	 	 	 	1.7366	 	 	 	1.9767	 	 	 	1.9060	 

Based on the Company’s foreign currency exposures noted above, varying the above
foreign exchange rates to reflect a 5% strengthening of the Canadian dollar would have
increased the net profit (loss) as follows, assuming that all other variables remained
constant:

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 
	 	 	2010	 	 	2009	 
	 
	 	 	$US	 	 	EURO	 	 	GBP	 	 	$US	 	 	Euro	 	 	GBP	 
	 
	Increase in net profit (loss)
	 	 	1,298	 	 	 	(1	)	 	 	(4	)	 	 	19	 	 	 	—	 	 	 	(1	)

	 	 	 	An assumed 5% weakening of the Canadian dollar would have had an equal but opposite
effect on the above currencies to the amounts shown above, assuming that all other
variables remain constant.
	 
	 	(d)	 	Interest rate risk:
	 
	 	 	 	Interest rate risk is the risk that the fair value or future cash flows of a financial
instrument will fluctuate because of changes in market interest rates.
	 
	 	 	 	Short-term bonds held by the Company are invested at fixed interest rates and/or mature in
the short-term. Long-term bonds are also instruments that bear interest at fixed rates. The
risk that the Company will realize a loss as a result of a decline in the fair value of its
bonds is limited because these investments, although they are classified as available for
sale, are generally held to maturity. The unrealized gains or losses on bonds are recorded
in accumulated other comprehensive income.

41

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	20.	 	Financial instruments (continued):
	 
	 	 	Overview (continued):

	 	(d)	 	Interest rate risk (continued):
	 
	 	 	 	Based on the value of the Company’s short and long-term bonds at November 30, 2010, an
assumed 0.5% decrease in market interest rates would have increased the fair value of these
bonds and the accumulated other comprehensive income by approximately $336; an assumed
increase in interest rate of 0.5% would have an equal but opposite effect, assuming that
all other variables remained constant.
	 
	 	 	 	Cash bears interest at a variable rate. Trade and other receivables, accounts payable and
accrued liabilities bear no interest.
	 
	 	 	 	Based on the average value of variable interest-bearing cash during the year ended November
30, 2010 ($3,219), an assumed 0.5% increase in interest rates during such period would have
increased future cash flow and net profit by approximately $16; an assumed decrease of 0.5%
would have had an equal but opposite effect.

	21.	 	Capital management:
	 
	 	 	The Company’s objective in managing capital is to ensure a sufficient liquidity position to
finance its research and development activities, general and administrative expenses, working
capital and capital spending.
	 
	 	 	To fund its activities, the Company relied primarily on public offerings of common shares in
Canada and private placements of its common shares as well as up-front payments and milestone
payments primarily associated with EMD Serono. When possible, the Company optimizes its
liquidity position using non-dilutive sources, including investment tax credits, grants and
interest income.
	 
	 	 	The Company has a $1,800 revolving credit facility for its short-term financing needs which was
unused at November 30, 2010 (see note 23 (c)).
	 
	 	 	The capital management objectives remain the same as for the previous year.
	 
	 	 	At November 30, 2010, cash and bonds amounted to $64,550 and tax credits and grants receivable
amounted to $332, for a total of $64,882. The Company believes that its cash position will be
sufficient to finance its operations and capital needs for the next year.
	 
	 	 	Currently, the Company’s general policy on dividends is to retain cash to keep funds available
to finance the Company’s growth.
	 
	 	 	The Company is not subject to any externally imposed capital requirements.

42

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	22.	 	Determination of fair values:
	 
	 	 	Certain of the Company’s accounting policies and disclosures require the determination of fair
value, for both financial and non-financial assets and liabilities. Fair values have been
determined for measurement and/or disclosure purposes based on the following methods. When
applicable, further information about the assumptions made in determining fair values is
disclosed in the notes specific to that asset or liability.
	 
	 	 	Financial assets and liabilities:
	 
	 	 	In establishing fair value, the Company uses a fair value hierarchy based on levels as defined
below:

	 	•	 	Level 1: defined as observable inputs such as quoted prices in active markets.
	 
	 	•	 	Level 2: defined as inputs other than quoted prices in active markets that are either
directly or indirectly observable.
	 
	 	•	 	Level 3: defined as inputs that are based on little or no observable market data,
therefore requiring entities to develop its own assumptions.

The Company has determined that the carrying values of its short-term financial assets and
liabilities, including cash, trade and other receivables as well as accounts payable and
accrued liabilities, approximate their fair value because of the relatively short period to
maturity of the instruments.

Bonds are stated at estimated fair value, determined by inputs that are primarily based on
broker quotes at the reporting date (Level 2).

Share-based payment transactions:

The fair value of the employee stock options is measured based on the Black-Scholes valuation
model. Measurement inputs include share price on measurement date, exercise price of the
instrument, expected volatility (based on weighted average historic volatility adjusted for
changes expected due to publicly available information), weighted average expected life of the
instruments (based on historical experience and general option holder behaviour), expected
dividends, and the risk-free interest rate (based on government bonds). Service and non-market
performance conditions attached to the transactions are not taken into account in determining
fair value.

43

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	23.	 	Commitments:

	 	(a)	 	Leases:
	 
	 	 	 	At November 30, 2010 and 2009 and December 1, 2008, the minimum payments required under the
terms of the non-cancellable lease are as follows:

	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 	 	December 1,	 
	 	 	2010	 	 	2009	 	 	2008	 
	 
	 	 	$	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Less than one year
	 	 	55	 	 	 	340	 	 	 	816	 
	Between one and five years
	 	 	2,239	 	 	 	2,020	 	 	 	340	 
	More than five years
	 	 	3,943	 	 	 	4,216	 	 	 	—	 
	 
	 
	 	 	6,237	 	 	 	6,576	 	 	 	1,156	 
	 

	 	(b)	 	Long-term procurement agreements:
	 
	 	 	 	During and after the years ended November 30, 2010 and 2009, the Company entered into
long-term procurement agreements with third-party suppliers in anticipation of the
commercialization of EGRIFTATM.
	 
	 	(c)	 	Credit facility:
	 
	 	 	 	The Company has a $1,800 revolving credit facility, bearing interest at prime plus 0.5%.
Under the term of the credit facility, the market value of investments held must always be
equivalent to 150% of amounts drawn under the facility. If the market value falls below
$7,000, the Company will provide the bank with a first rank movable hypothec (security
interest) of $1,850 on securities judged satisfactory by the bank.
	 
	 	 	 	As at November 30, 2010 and 2009, the Company did not have any borrowings outstanding under
this credit facility.

	24.	 	Operating segments:
	 
	 	 	The Company has a single operating segment. As described in note 4, all of the Company’s
revenues are generated from one customer, EMD Serono, which is domiciled in the United States.
	 
	 	 	All of the Company’s non-current assets are located in Canada, the Company’s headquarters.

44

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	25.	 	Related parties:
	 
	 	 	The Company has a related party relationship with its wholly-owned subsidiaries. There are no
transactions between the Company and its subsidiaries.
	 
	 	 	The key management personnel of the Company are the Directors.
	 
	 	 	Key management personnel compensation comprised:

	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	November 30,	 	 	November 30,	 
	 	 	Note	 	 	2010	 	 	2009	 
	 
	 	 	 	 	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Short-term employee benefits
	 	 	 	 	 	 	1,891	 	 	 	1,647	 
	Post-employment benefits
	 	 	 	 	 	 	61	 	 	 	59	 
	Share-based compensation
	 	15 (iv)	 	 	331	 	 	 	175	 
	 
	 
	 	 	 	 	 	 	2,283	 	 	 	1,881	 
	 

	 	 	Directors of the Company control 1.2 percent of the voting shares of the Company.
	 
	 	 	On November 30, 2010, loans granted to key management personnel under share purchase plan (note
15 (iii)) amount to $22 as at November 30, 2010 ($75 as at November 30, 2009 and $59 as at
December 1, 2008).
	 
	26.	 	Subsequent events:
	 
	 	 	Distribution and licensing agreement:
	 
	 	 	On December 6, 2010, the Company announced the signing of a distribution and licensing
agreement with Sanofi-aventis (“Sanofi”), covering the commercial rights for EGRIFTATM in
Latin America, Africa, and the Middle East for the treatment of excess abdominal fat in
HIV-infected patients with lipodystrophy.
	 
	 	 	Under the terms of the agreement, the Company will sell EGRIFTATM to Sanofi at a transfer price
equal to the higher of a percentage of Sanofi’s net selling price and a predetermined floor
price. The Company has retained all future development rights to EGRIFTATM and will be
responsible for conducting research and development for any additional potential indications.
Sanofi will be responsible for conducting all regulatory activities for EGRIFTATM in the
aforementioned territories, including applications for approval in the different countries for
the treatment of excess abdominal fat in HIV-infected patients with lipodystrophy. The Company
also granted Sanofi an option to commercialize tesamorelin for other indications in the
territories mentioned above. If such option is not exercised, or is declined, by Sanofi, the
Company may commercialize tesamorelin for such indications on its own or with a third party.

45

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts)

 

	26.	 	Subsequent events (continued):
	 
	 	 	Distribution and licensing agreement (continued):
	 
	 	 	On February 3, 2011, the Company entered into a distribution and licensing agreement with
Ferrer covering the commercial rights for EGRIFTATM for the treatment of
excess abdominal fat in HIV-infected patients with lipodystrophy in Europe, Russia, South
Korea, Taiwan, Thailand and certain central Asian countries.
	 
	 	 	Under the terms of the Agreement, the Company will sell EGRIFTATM to
Ferrer at a transfer price equal to the higher of a significant percentage of the Ferrer’s net
selling price and a predetermined floor price. The Company has retained all development rights
to EGRIFTATM for other indications and will be responsible for
conducting research and development for any additional programs. Ferrer will be responsible for
conducting all regulatory and commercialization activities in connection with
EGRIFTATM for the treatment of excess abdominal fat in HIV-infected
patients with lipodystrophy in the territories subject to the agreement. The Company will be
responsible for the manufacture and supply of EGRIFTATM to Ferrer. The
Company has the option to co-promote EGRIFTATM for the reduction of
excess abdominal fat in HIV-infected patients with lipodystrophy in the territories. Ferrer has
the option to enter into a co-development and commercialization agreement using tesamorelin
relating to any such new indications. The terms and conditions of such a co-development and
commercialization agreement will be negotiated based on any additional program chosen for
development.
	 
	 	 	Deferred share unit plan:
	 
	 	 	In December 2010, the Company adopted a deferred share unit plan (“Plan”) to provide
long-term incentive compensation for its directors and executive officers. Under the Plan,
directors must receive their annual remuneration as a board member in fully vested deferred
share units (“DSUs”) until they reach a percentage of their annual remuneration and, once
such percentage is attained, they have the option to elect to receive part or all of this
annual remuneration in DSUs. Under the plan, executive officers have the option of receiving
all or a portion of their annual bonus in the form of fully-vested DSUs. The units are only
redeemable for cash when a participant ceases to be an employee or member of the Board of
Directors. The Company manages the risk associated with the issuance of the DSU by entering
into a yearly forward contract with a third party. As at February 7, 2011, all of the 99,912
DSU outstanding were covered by a prepaid forward contract.
	 
	 	 	Stock option plan:
	 
	 	 	Between December 1, 2010 and February 7, 2011, the Company granted 250,000 options at an
exercise price of $5.65 per share. Also 27,832 options were forfeited and expired at a weighted
exercise average price of $12.06 per share. Furthermore, 3,000 options were exercised at a
weighted exercise average price of $1.80 per share for a cash consideration of $5.

46

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	27.	 	Transition to IFRS:
	 
	 	 	As stated in note 2 (a), these are the Company’s first consolidated financial statements
prepared in accordance with IFRSs. The Company has applied IFRS 1 and the accounting policies
set out in note 3 in preparing the financial statements for the year ended November 30, 2010,
the comparative information presented in these financial statements for the year ended November
30, 2009 and in the opening IFRS statement of financial position at December 1, 2008 (the
Company’s date of transition).
	 
	 	 	In preparing these consolidated financial statements in accordance with IFRS 1, the Company has
applied the mandatory exceptions and certain of the optional exemptions from full retrospective
application of IFRSs.
	 
	 	 	The Company elected to apply the following optional exemptions from full retrospective
application:

	 	(i)	 	Share-based payment transaction exemption:
	 
	 	 	 	The Company has elected to apply the share-based payment exemption. It applied IFRS 2 from
December 1, 2008 to those stock options that were issued after November 7, 2002 but that
had not vested by December 1, 2008. The application of the exemption is detailed below.
	 
	 	(ii)	 	Designation of financial assets and financial liabilities exemption:
	 
	 	 	 	The Company elected to re-designate cash from the held-for-trading category to loans and
receivables.

	 	 	As required by IFRS 1, estimates made under IFRS at the date of transition must be consistent
with estimates made for the same date under previous GAAP, unless there is evidence that those
estimates were in error.
	 
	 	 	In preparing its opening IFRS consolidated statement of financial position, the Company has
adjusted amounts reported previously in financial statements prepared in accordance with
Canadian GAAP.
	 
	 	 	An explanation of how the transition from previous Canadian GAAP to IFRS has affected the
Company’s financial position, financial performance and cash flows is set out in the following
tables and accompanying notes.

47

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	27.	 	Transition to IFRS (continued):
	 
	 	 	Reconciliation of equity as at December 1, 2008 and November 30, 2009:

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	December 1, 2008	 	 	November 30, 2009	 
	 	 	 	 	 	 	 	 	 	 	IFRS	 	 	IFRS	 	 	 	 	 	 	 	 	 	 	IFRS	 	 	IFRS	 	 	 	 
	 	 	 	 	 	 	Canadian	 	 	adjust-	 	 	reclassi-	 	 	 	 	 	 	Canadian	 	 	adjust-	 	 	reclassi-	 	 	 	 
	 	 	Note	 	 	GAAP	 	 	ments	 	 	fications	 	 	IFRS	 	 	GAAP	 	 	ments	 	 	fications	 	 	IFRS	 
	 	 	 	 	 	 	$	 	 	$	 	 	$	 	 	$	 	 	$	 	 	$	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Assets
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Current assets:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Cash
	 	 	 	 	 	 	133	 	 	 	—	 	 	 	—	 	 	 	133	 	 	 	1,519	 	 	 	—	 	 	 	—	 	 	 	1,519	 
	Bonds
	 	 	 	 	 	 	10,955	 	 	 	—	 	 	 	—	 	 	 	10,955	 	 	 	10,036	 	 	 	—	 	 	 	—	 	 	 	10,036	 
	Trade and other
receivables
	 	 	 	 	 	 	610	 	 	 	—	 	 	 	—	 	 	 	610	 	 	 	375	 	 	 	—	 	 	 	—	 	 	 	375	 
	Tax credits and
grants receivable
	 	 	(a	)	 	 	1,784	 	 	 	—	 	 	 	(333	)	 	 	1,451	 	 	 	1,666	 	 	 	—	 	 	 	(333	)	 	 	1,333	 
	Inventories
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	2,225	 	 	 	—	 	 	 	—	 	 	 	2,225	 
	Research supplies
	 	 	(a	)	 	 	301	 	 	 	—	 	 	 	(301	)	 	 	—	 	 	 	287	 	 	 	—	 	 	 	(287	)	 	 	—	 
	Prepaid expenses
	 	 	(a	)	 	 	397	 	 	 	—	 	 	 	342	 	 	 	739	 	 	 	302	 	 	 	—	 	 	 	328	 	 	 	630	 
	 
	Total current assets
	 	 	 	 	 	 	14,180	 	 	 	—	 	 	 	(292	)	 	 	13,888	 	 	 	16,410	 	 	 	—	 	 	 	(292	)	 	 	16,118	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Non-current assets:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Bonds
	 	 	 	 	 	 	35,249	 	 	 	—	 	 	 	—	 	 	 	35,249	 	 	 	51,807	 	 	 	—	 	 	 	—	 	 	 	51,807	 
	Property and equipment
	 	 	 	 	 	 	1,299	 	 	 	—	 	 	 	—	 	 	 	1,299	 	 	 	1,229	 	 	 	—	 	 	 	—	 	 	 	1,229	 
	Other assets
	 	 	(a	)	 	 	2,817	 	 	 	—	 	 	 	(41	)	 	 	2,776	 	 	 	41	 	 	 	—	 	 	 	(41	)	 	 	—	 
	 
	Total non-current assets
	 	 	 	 	 	 	39,365	 	 	 	—	 	 	 	(41	)	 	 	39,324	 	 	 	53,077	 	 	 	—	 	 	 	(41	)	 	 	53,036	 
	 
	Total assets
	 	 	 	 	 	 	53,545	 	 	 	—	 	 	 	(333	)	 	 	53,212	 	 	 	69,487	 	 	 	—	 	 	 	(333	)	 	 	69,154	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Liabilities
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Current liabilities:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Accounts payable
and accrued liabilities
	 	 	(a	)	 	 	7,198	 	 	 	—	 	 	 	(333	)	 	 	6,865	 	 	 	5,901	 	 	 	—	 	 	 	(333	)	 	 	5,568	 
	Current portion of
deferred revenue
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	6,847	 	 	 	—	 	 	 	—	 	 	 	6,847	 
	 
	Total current liabilities
	 	 	 	 	 	 	7,198	 	 	 	—	 	 	 	(333	)	 	 	6,865	 	 	 	12,748	 	 	 	—	 	 	 	(333	)	 	 	12,415	 
	 
	Non-current liabilities:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Deferred revenue
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	13,691	 	 	 	—	 	 	 	—	 	 	 	13,691	 
	 
	Total non-current liabilities
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	—	 	 	 	13,691	 	 	 	—	 	 	 	—	 	 	 	13,691	 
	 
	Total liabilities
	 	 	 	 	 	 	7,198	 	 	 	—	 	 	 	(333	)	 	 	6,865	 	 	 	26,439	 	 	 	—	 	 	 	(333	)	 	 	26,106	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Equity
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Share capital
	 	 	 	 	 	 	269,219	 	 	 	—	 	 	 	—	 	 	 	269,219	 	 	 	279,169	 	 	 	—	 	 	 	—	 	 	 	279,169	 
	Contributed surplus
	 	 	(b	)	 	 	5,585	 	 	 	175	 	 	 	—	 	 	 	5,760	 	 	 	6,484	 	 	 	273	 	 	 	—	 	 	 	6,757	 
	Deficit
	 	 	(b	)	 	 	(228,829	)	 	 	(175	)	 	 	—	 	 	 	(229,004	)	 	 	(243,887	)	 	 	(273	)	 	 	—	 	 	 	(244,160	)
	Accumulated other
comprehensive income
	 	 	 	 	 	 	372	 	 	 	—	 	 	 	—	 	 	 	372	 	 	 	1,282	 	 	 	—	 	 	 	—	 	 	 	1,282	 
	 
	Total equity
	 	 	 	 	 	 	46,347	 	 	 	—	 	 	 	—	 	 	 	46,347	 	 	 	43,048	 	 	 	—	 	 	 	—	 	 	 	43,048	 
	 
	Total liabilities and equity
	 	 	 	 	 	 	53,545	 	 	 	—	 	 	 	(333	)	 	 	53,212	 	 	 	69,487	 	 	 	—	 	 	 	(333	)	 	 	69,154	 
	 

48

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	27.	 	Transition to IFRS (continued):
	 
	 	 	Reconciliation of comprehensive income for the year ended November 30, 2009:

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	IFRS	 	 	IFRS	 	 	 	 
	 	 	 	 	 	 	Canadian	 	 	adjust-	 	 	reclassi-	 	 	 	 
	 	 	Note	 	 	GAAP	 	 	ments	 	 	fication	 	 	IFRS	 
	 	 	 	 	 	 	$	 	 	$	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Revenue:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Research services:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Milestone payments
	 	 	(c	)	 	 	—	 	 	 	—	 	 	 	10,884	 	 	 	10,884	 
	Upfront payments and initial technology access fees
	 	 	(c	)	 	 	—	 	 	 	—	 	 	 	6,560	 	 	 	6,560	 
	Royalties and license fees
	 	 	(c	)	 	 	17,468	 	 	 	—	 	 	 	(17,444	)	 	 	24	 
	Interest
	 	 	(c	)	 	 	2,252	 	 	 	—	 	 	 	(2,252	)	 	 	—	 
	 
	Total revenue
	 	 	 	 	 	 	19,720	 	 	 	—	 	 	 	(2,252	)	 	 	17,468	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Research and development expenses, net of tax credits
	 	 	(b), 	(c)	 	 	20,431	 	 	 	33	 	 	 	346	 	 	 	20,810	 
	Selling and market development expenses
	 	 	(b), 	(c)	 	 	2,583	 	 	 	10	 	 	 	4,269	 	 	 	6,862	 
	General and administrative expenses
	 	 	(b), 	(c)	 	 	7,149	 	 	 	55	 	 	 	(661	)	 	 	6,543	 
	Patents
	 	 	(c	)	 	 	346	 	 	 	—	 	 	 	(346	)	 	 	—	 
	Fees associated with the collaboration and licensing
agreement
	 	 	(c	)	 	 	4,269	 	 	 	—	 	 	 	(4,269	)	 	 	—	 
	 
	Total operating expenses
	 	 	 	 	 	 	34,778	 	 	 	98	 	 	 	(661	)	 	 	34,215	 
	 
	Results from operating activities
	 	 	 	 	 	 	(15,058	)	 	 	(98	)	 	 	(1,591	)	 	 	(16,747	)
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Finance income
	 	 	(c	)	 	 	—	 	 	 	—	 	 	 	2,252	 	 	 	2,252	 
	Finance costs
	 	 	(c	)	 	 	—	 	 	 	—	 	 	 	(661	)	 	 	(661	)
	 
	Total net finance income
	 	 	 	 	 	 	—	 	 	 	—	 	 	 	1,591	 	 	 	1,591	 
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Net loss
	 	 	 	 	 	 	(15,058	)	 	 	(98	)	 	 	—	 	 	 	(15,156	)
	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Other comprehensive income:
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Net change in fair value of available-for-sale financial assets
	 	 	 	 	 	 	1,039	 	 	 	—	 	 	 	—	 	 	 	1,039	 
	Net change in fair value of available-for-sale financial assets
transferred to net profit (loss)
	 	 	 	 	 	 	(129	)	 	 	—	 	 	 	—	 	 	 	(129	)
	 
	Other comprehensive income for the year
	 	 	 	 	 	 	910	 	 	 	—	 	 	 	—	 	 	 	910	 
	 
	Total comprehensive income for the year
	 	 	 	 	 	 	(14,148	)	 	 	(98	)	 	 	—	 	 	 	(14,246	)
	 

	 	 	Material adjustments to the consolidated statement of cash flows for 2009:
	 
	 	 	There are no material differences between the consolidated statement of cash flows presented
under IFRS and the consolidated statement of cash flows presented under previous Canadian GAAP.

49

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	27.	 	Transition to IFRS (continued):
	 
	 	 	Notes to the reconciliations:

	 	(a)	 	Reclassification in the consolidated statement of financial position:
	 
	 	 	 	Certain corresponding figures as at December 1, 2008 and November 30, 2009 have been
reclassified to conform to the new presentation under IFRS.
	 
	 	(b)	 	Share-based compensation:
	 
	 	 	 	In certain situations, stock options granted vest in instalments over a specified vesting
period. When the only vesting condition is service from the grant date to the vesting date
of each tranche awarded, then each instalment should be accounted for as a separate
share-based payment arrangement under IFRS, otherwise known as graded vesting. Canadian
GAAP permits an entity the accounting policy choice with respect to graded vesting awards.
Each instalment can be considered as a separate award, each with a different vesting
period, consistent with IFRS, or the arrangement can be treated as a single award with a
vesting period based on the average vesting period of the instalments depending on the
policy elected.
	 
	 	 	 	The Company’s policy under Canadian GAAP was to treat graded vesting awards under the
latter method and, as a result, an adjustment of $175 was required on the application of
IFRS 2 at the transition date, and an adjustment of $98 was required for the restated 2009
comparative balances as shown below:

	 	 	 	 	 	 	 	 	 
	 	 	December 1,	 	 	November 30,	 
	 	 	2008	 	 	2009	 
	 	 	$	 	 	$	 
	 
	 	 	 	 	 	 	 	 
	Consolidated statement of comprehensive income:
	 	 	 	 	 	 	 	 
	Increase in research and development expenses
	 	 	—	 	 	 	33	 
	Increase in selling and market development expenses
	 	 	—	 	 	 	10	 
	Increase in general and administrative expenses
	 	 	—	 	 	 	55	 
	 
	 
	 	 	 	 	 	 	 	 
	Adjustment to net loss and total comprehensive loss
	 	 	—	 	 	 	98	 
	 
	 
	 	 	 	 	 	 	 	 
	Deficit
	 	 	(175	)	 	 	(273	)
	Increase in contributed surplus
	 	 	175	 	 	 	273	 
	 

50

 

THERATECHNOLOGIES INC.

Notes to the Consolidated Financial Statements, Continued

Years ended November 30, 2010 and 2009 and as at December 1, 2008

(in thousands of Canadian dollars, except per share amounts) 

	27.	 	Transition to IFRS (continued):
	 
	 	 	Notes to the reconciliations (continued):

	 	(c)	 	Reclassification in the consolidated statement of comprehensive income:
	 
	 	 	 	Under IFRS, the Company elected to present expenses using a classification based on their
function and presents net finance income separately. The effect of these changes is
summarized below:

	 	 	 	 	 
	 	 	November 30,	 
	 	 	2009	 
	 	 	$	 
	Decrease in interest
	 	 	(2,252	)
	Increase in finance income
	 	 	2,252	 
	Increase in research and development expenses
	 	 	346	 
	Decrease in patent fees
	 	 	(346	)
	Decrease in general and administrative expenses
	 	 	(661	)
	Increase in finance costs
	 	 	661	 
	Increase in selling and market development expenses
	 	 	4,269	 
	Decrease in fees associated with the collaboration and licensing agreement
	 	 	(4,269	)
	 
	 
	 	 	—	 
	 

	 	 	 	Changes in presentation were also made to the revenue caption in order to conform with
the new presentation under IFRS as noted below:

	 	 	 	 	 
	 	 	November 30,	 
	 	 	2009	 
	 	 	$	 
	Decrease in royalties and license fees
	 	 	(17,444	)
	Increase in upfront payments and initial technology access fees
	 	 	6,560	 
	Increase in milestone payments
	 	 	10,884	 
	 
	 
	 	 	—	 
	 
	 	 	 
	 

51EX-4.3

Exhibit 4.3

Forward-Looking Information

This Management’s discussion and analysis (“MD&A”) contains certain statements that are considered
“forward-looking information” within the meaning of applicable securities legislation. This
forward-looking information includes, but is not limited to, information regarding the preparation
and filing of applications seeking regulatory approval of EGRIFTATM in the treatment of
excess abdominal fat in HIV-infected patients with lipodystrophy in various territories outside of
the United States, the revenue to be generated as a result of sales of EGRIFTATM to EMD
Serono, Inc., (“EMD Serono”), the receipt of royalties from EMD Serono in connection with the sale
of EGRIFTATM in the United States, and the development of tesamorelin in a new clinical
program for a new indication. Furthermore, the words “will”, “may”, “could”, “should”, “outlook”,
“believe”, “plan”, “envisage”, “anticipate”, “expect” and “estimate”, or the negatives of these
terms or variations of them and the use of future or conditional tenses as well as similar
expressions denote forward-looking information.

Forward-looking information is based upon a number of assumptions and is subject to a number of
risks and uncertainties, many of which are beyond the Company’s control, that could cause actual
results to differ materially from those that are disclosed in or implied by such forward-looking
information. These risks and uncertainties are described under the section “Risks and
Uncertainties” on page 21 and include, but are not limited to, the risk that EGRIFTATM
is not approved in all or some of the territories referred to in this MD&A, the revenue and
royalties we expect to generate from sales of EGRIFTATM is lower than anticipated, the
supply of EGRIFTATM to our commercial partners is delayed or suspended as a result of
problems with our suppliers, EGRIFTATM is withdrawn from the market as a result of
defects or recalls, our intellectual property is not adequately protected and our liquidity level
decreases based on unexpected activities that must be carried out in order to achieve our business
plan.

Although the forward-looking information contained in this MD&A is based upon what we believe are
reasonable assumptions, investors are cautioned against placing undue reliance on this information
since actual results may vary materially from the forward-looking information contained in this
MD&A. Certain assumptions made in preparing the forward-looking information include the assumption
that tesamorelin for the reduction of excess abdominal fat in HIV-infected patients with
lipodystrophy will receive approval in the territories referred to in this MD&A, no additional
clinical studies will be required to obtain said regulatory approval of tesamorelin,
EGRIFTATM will be accepted by the marketplace in the United States and will be on the
list of reimbursed drugs by third-party payers, our relations with third-party suppliers of
EGRIFTATM will be conflict-free and that such third-party suppliers will have enough
capacity to manufacture and supply EGRIFTATM to meet its demand and on a timely-basis
and that our business plan will not be substantially modified.

Consequently, all of the forward-looking information contained in this MD&A is qualified by the
foregoing cautionary statements, and there can be no guarantee that the results or developments
that we anticipate will be realized or, even if substantially realized, that they will have the
expected consequences or effects on our business, financial condition or results of operation.

 

 

Management’s Discussion and Analysis

The following discussion and analysis provides management’s point of view on the financial position
and the results of operations of Theratechnologies Inc., on a consolidated basis for the
twelve-month periods ended November 30, 2010 (“fiscal 2010”) and November 30, 2009 (“fiscal 2009”).
Unless otherwise indicated or unless the context requires otherwise, all references in this MD&A to
“Theratechnologies”, “the Company”, “we”, “us”, “our” or similar terms refer to Theratechnologies
Inc. and its consolidated subsidiaries. This information is dated February 8, 2011, and should be
read in conjunction with the Audited Consolidated Financial Statements and the accompanying notes.
Unless specified otherwise, all amounts are in Canadian dollars. In this MD&A, the use of
“EGRIFTATM” refers to tesamorelin for the reduction of excess abdominal fat in
HIV-infected patients with lipodystrophy regardless of the trade name used for such product in any
particular territory. EGRIFTATM is the trade name used in the United States for
tesamorelin for the reduction of excess abdominal fat in HIV-infected patients with lipodystrophy.

Except as otherwise indicated, the financial information contained in this MD&A and in our Audited
Consolidated Financial Statements has been prepared in accordance with International Financial
Reporting Standards (“IFRS”) as issued by the International Accounting Standards Board (“IASB”).

Our financial statements were previously prepared in accordance with Canadian Generally Accepted
Accounting Principles (“GAAP”). For more information regarding the conversion to IFRS, please refer
to the heading “Conversion to IFRS” in this MD&A and to note 27 of the Audited Consolidated
Financial Statements, which are our first consolidated financial statements prepared in accordance
with IFRS.

The Audited Consolidated Financial Statements and MD&A have been reviewed by our Audit Committee
and approved by our Board of Directors.

Overview

We are a specialty pharmaceutical company that discovers and develops innovative therapeutic
peptide products with an emphasis on growth-hormone releasing factor peptides. We are leveraging
our expertise in the field of metabolism to discover and develop products in specialty markets. Our
commercialization strategy is to retain all or a significant portion of the commercial rights to
our products. Our first product, EGRIFTATM (tesamorelin for injection), was approved by the United
States Food and Drug Administration (“FDA”) in November 2010. To date, EGRIFTATM is the only
approved therapy for the reduction of excess abdominal fat in HIV-infected patients with
lipodystrophy.

Lipodystrophy in HIV-infected patients presents a serious medical condition, affecting
approximately 29% of all diagnosed and treated HIV-infected patients. This condition is associated
with a range of physiological and psychological complications beyond the significant health and
mortality risks of the HIV infection itself. EGRIFTATM is currently marketed in the United States by
EMD Serono, Inc. (“EMD Serono”), an affiliate of Merck KGaA, pursuant to a collaboration and
licensing agreement entered into by us and EMD Serono in October 2008. In addition, we have signed
distribution and licensing agreements with Sanofi Winthrop Industries, an affiliate of
Sanofi-aventis (collectively, “Sanofi”), for the commercialization rights for EGRIFTATM for the
reduction of excess abdominal fat in HIV-infected patients with lipodystrophy in Latin America,
Africa and the Middle East and with Ferrer Internacional S.A. (“Ferrer”) for the commercialization
rights for EGRIFTATM for the reduction of excess abdominal fat in HIV-

- 2 - 

 

infected patients with lipodystrophy in Europe, Russia, South Korea, Taiwan, Thailand and certain
central Asian countries. EGRIFTATM is the trade name used in the United States for tesamorelin for
the reduction of excess abdominal fat in HIV-infected patients with lipodystrophy.

The first six months of fiscal 2010 were devoted to preparing for a public meeting with the
Endocrinologic and Metabolic Drugs Advisory Committee, which the FDA of the United States had asked
us to attend in the context of its review of our New Drug Application (“NDA”) for EGRIFTATM. As an
integral part of the FDA review process for a NDA, the principal role of an advisory committee is
to provide an independent point of view to enhance the quality of the agency’s regulatory
decision-making process. At the public meeting held on May 27, 2010, the committee of experts
unanimously recommended to the FDA, the approval of EGRIFTATM.

In the second half of fiscal 2010, we focused primarily on responding to the FDA’s questions and
began building our inventory in anticipation of the launch of EGRIFTATM in the United States. We
were also focused on securing strategic alliances for the commercialization of EGRIFTATM in
territories outside of the United States.

On November 10, 2010, the FDA approved EGRIFTATM as the first approved treatment in the United
States for the reduction of excess abdominal fat in HIV-infected patients with lipodystrophy. By
virtue of the collaboration and licensing agreement entered into in 2008 with EMD Serono, we
received a milestone payment of US$25,000,000 associated with the FDA-approval of EGRIFTATM. This
payment was received by us on November 30, 2010. Under the collaboration and licensing agreement,
EMD Serono has the exclusive right to commercialize EGRIFTATM in the United States for
the reduction of excess abdominal fat in HIV-infected patients with lipodystrophy.

Concurrent with these regulatory activities in fiscal 2010, our third-party suppliers began
manufacturing inventory of EGRIFTATM in preparation for the launch of EGRIFTATM in the United States
by our commercial partner, EMD Serono. The first product shipment of EGRIFTATM took place in
December 2010.

Fiscal 2010 was also marked by a change in our management. On December 1, 2010, John-Michel T.
Huss, previously Chief of Staff, Office of the CEO, of Sanofi in Paris, became our President and
Chief Executive Officer. Mr. Huss replaced Yves Rosconi who, in June 2010, announced his desire to
retire after six years as the head of the Company.

On December 6, 2010, we entered into a distribution and licensing agreement with Sanofi granting
them the exclusive commercialization rights of EGRIFTATM for the treatment of excess
abdominal fat in HIV-infected patients with lipodystrophy in Latin America, Africa and the Middle
East.

On February 3, 2011, we entered into a distribution and license agreement with Ferrer granting them
the exclusive commercialization rights of tesamorelin for the treatment of excess abdominal fat in
HIV-infected patients with lipodystrophy in Europe, Russia, South Korea, Taiwan, Thailand and
certain central Asian countries.

Financial Position

We completed fiscal 2010 with a liquidity position of $64,882,000, consisting of $64,550,000 of
cash and highly liquid bonds, and $332,000 of tax credits and grants receivable.

- 3 - 

 

Economic Environment

In 2008 and 2009, capital markets were characterized by significant stock market volatility and a
notable decline in access to capital, particularly for the biotechnology industry. An economic
slowdown occurred in almost all sectors and the general decline of the capital markets had a
negative effect on the cost of capital for companies.

In early 2010, the situation remained challenging and it was only in the second half of the year
that we began to see an improvement in economic conditions, which resulted in better access to
capital and lower credit risk. Interest rates, however, remained extremely low throughout the year.

Despite the improvement in general market conditions, our investment policy continues to be
conservative. We have invested our funds in highly liquid, low-risk instruments as described under
the heading “Liquidity and capital resources”.

Perspectives for 2011

In 2011, our focus is to maximize the global opportunities for EGRIFTATM and
tesamorelin. In order to do so we intend to:

	 	•	 	Support our commercial partner, EMD Serono, in commercializing EGRIFTATM
in the United States;
	 
	 	•	 	Support our commercial partner, Sanofi, in seeking regulatory approval of
EGRIFTATM in Latin America, Africa and the Middle-East for potential
commercialization;
	 
	 	•	 	Support our commercial partner, Ferrer, in seeking regulatory approval of
EGRIFTATM in Europe, Russia, South Korea, Taiwan, Thailand and certain central
Asian countries for potential commercialization;
	 
	 	•	 	Assess expansion opportunities into other territories where EGRIFTATM
could be used for the reduction of excess abdominal fat in HIV-infected patients with
lipodystrophy;
	 
	 	•	 	Initiate a new clinical program evaluating tesamorelin in a new indication;
	 
	 	•	 	Continue working on EGRIFTATM. We have developed a new presentation of
EGRIFTATM which is easier to use than its current presentation. This new
presentation complies with one of the FDA’s post-approval requirements. See “Post-Approval
Commitments”; and
	 
	 	•	 	Develop a new formulation for EGRIFTATM pursuant to our agreement with EMD
Serono.

- 4 - 

 

Selected Annual Information

	 	 	 	 	 	 	 	 	 	 	 	 	 
	Consolidated statement of comprehensive income	 	 	 	 	 	 
	YEARS ENDED NOVEMBER 30 (in thousands of	 	 	 	 	 	 
	Canadian dollars, except per share amounts)	 	2010	 	2009	 	2008(1)
	 
	Revenue(2)
	 	$	31,868	 	 	$	17,468	 	 	$	2,641	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Research and development expenses, net of tax
credits
	 	$	14,064	 	 	$	20,810	 	 	$	33,215	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Results from operating activities
	 	$	6,663	 	 	$	(16,747	)	 	$	(48,611	)
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Net financial income
	 	$	2,381	 	 	$	1,591	 	 	 	—	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Net profit (loss)
	 	$	8,930	 	 	$	(15,156	)	 	$	(48,611	)
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Basic and diluted earnings (loss) per share
	 	$	0.15	 	 	$	(0.25	)	 	$	(0.85	)

	 	 	 	 	 	 	 	 	 	 	 	 	 
	Consolidated statement of financial position	 	 	 	 	 	 
	AT NOVEMBER 30 (in thousands of Canadian	 	 	 	 	 	 
	dollars)	 	2010	 	2009	 	2008(1)
	 
	Liquidities (cash and bonds)
	 	$	64,550	 	 	$	63,362	 	 	$	46,337	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Tax credits and grants receivable
	 	$	332	 	 	$	1,333	 	 	$	1,784	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Total assets
	 	$	71,651	 	 	$	69,154	 	 	$	53,545	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Total share capital
	 	$	279,398	 	 	$	279,169	 	 	$	269,219	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	Total equity
	 	$	52,656	 	 	$	43,048	 	 	$	46,347	 

 

			
	(1)	 	We adopted IFRS in fiscal 2010 with a transition date of December 1, 2008.
Consequently, the selected financial information for the year ended November 30, 2008, as presented
in our 2009 Audited Consolidated Financial Statements, which were presented in conformity with
Canadian GAAP, was not restated in terms of IFRS and accordingly, is not comparable with the
information for fiscal 2010 and 2009. See “Conversion to IFRS” for the policy differences between
Canadian GAAP and IFRS.
	 
	(2)	 	Revenue in 2008 includes interest income of $2,427,000. Revenue in 2009 includes a
milestone payment of $10,884,000 received from EMD Serono following the FDA’s acceptance to file
our NDA for EGRIFTATM. Revenue in 2010 includes a milestone payment of $25,000,000
received from EMD Serono following marketing approval of EGRIFTATM by the FDA.

- 5 - 

 

Operating Results

Revenue

Our consolidated revenue for the year ended November 30, 2010 was $31,868,000, compared to
$17,468,000 in 2009. The increased revenue in fiscal 2010 was related to the milestone payment of
US$25,000,000 (C$25,000,000) received by us from EMD Serono on November 30, 2010 associated with
the satisfaction of the condition of approval of EGRIFTATM by the FDA. In fiscal 2009, a
payment of US$10,000,000 (C$10,884,000) was received by us from EMD Serono following the acceptance
by the FDA of the Company’s NDA for EGRIFTATM in conformity with the collaboration and
licensing agreement with EMD Serono.

The initial payment of US$22,000,000 (C$27,097,000) received on December 15, 2008, upon the closing
of the transaction with EMD Serono, has been deferred and is being amortized over its estimated
service period of four years on a straight-line basis. For the year ended November 30, 2010, an
amount of $6,846,000 related to this transaction was recognized as revenue. At November 30, 2010,
the deferred revenue related to this transaction recorded on the consolidated statement of
financial position amounted to $13,692,000.

We expect to generate revenue from sales of EGRIFTATM to EMD Serono throughout fiscal
2011. We also expect to receive royalties on sales of EGRIFTATM in the United States by
EMD Serono beginning in the second quarter of fiscal 2011 upon receipt and confirmation of the
sales report relating to the previous quarter. The royalty rate we receive from EMD Serono is based
on the level of annual net sales achieved, with the rate increasing as higher levels of net sales
are attained.

R&D Activities

For the year ended November 30, 2010, consolidated research and development (“R&D”) expenses, net
of tax credits, amounted to $14,064,000, compared to $20,810,000 in 2009, a decrease of 32.4%. The
majority of R&D expenses incurred in fiscal 2010 are related to follow-up on work derived from the
regulatory filing with the FDA, notably responding to the FDA’s questions, and preparation for the
FDA Advisory Committee meeting. In parallel with the United States FDA review, we continued to
advance our regulatory filing in Europe and to work on a new presentation of the existing
formulation of EGRIFTATM. Furthermore, we are in the process of evaluating the
initiation of a new clinical program to develop tesamorelin for a new indication. In our discovery
and preclinical groups, we continued to develop new peptides and to advance our preclinical program
for acute kidney injury (“AKI”). In fiscal 2009, the expenses incurred were principally associated
with completing the Phase 3 clinical trials evaluating tesamorelin in HIV-associated lipodystrophy
and the preparation of the NDA, which was submitted to the FDA in May 2009. The significant decline
in R&D expenses was in accordance with our projected R&D expenses for fiscal 2010. We expect the
amount of our R&D expenses for fiscal 2011 to be similar to those of 2010.

Cost of Sales

In fiscal 2010, we began producing through our third-party suppliers inventories in anticipation of
the launch of EGRIFTATM in the United States. Cost of sales in fiscal 2010 related to
this activity amounted to $469,000 which includes a charge of $192,000, in order to value the
inventories at their net realizable value. This write-down was due to raw materials that were not
originally bought under the conditions of our current long-term procurement agreements. Cost of
sales also included unallocated costs related to the production fees associated with the start-up
of the manufacturing process. We expect the cost of sales to increase significantly over the next
fiscal

- 6 - 

 

year as sales of EGRIFTATM grow and as we secure additional suppliers for raw materials
and finished products.

General and Administrative Expenses

For the year ended November 30, 2010, general and administrative expenses were $8,002,000, compared
to $6,543,000 for the same period in fiscal 2009.

The higher expenses for the year ended November 30, 2010 are primarily due to the cost and expenses
associated with professional fees for the recruitment of the new President and Chief Executive
Officer, increased corporate communication associated with the FDA Advisory Committee meeting and
FDA approval, and conversion of our financial statements to IFRS, as well as costs and expenses
related to variations in share-based compensation expenses. The expenses for the year ended
November 30, 2009 include the costs associated with the revision of our three-year business plan
which were not repeated in fiscal 2010.

Selling and Market Development Expenses

For the year ended November 30, 2010, selling and market development expenses were $2,670,000,
compared to $6,862,000 in fiscal 2009.

The selling and market development expenses in fiscal 2010 are principally composed of business
development expenses and market research outside the United States and the costs of managing the
agreement with EMD Serono. In
fiscal 2009, we incurred expenses totaling $4,269,000 in connection with professional fees related
to the transaction with EMD Serono.

Net Financial Income

For the year ended November 30, 2010, interest income was $1,562,000 compared to $2,123,000 in
fiscal 2009. The year-over-year decline is due to lower average cash positions and a decrease in
yield on our bond portfolio. Receipt of the $25,000,000 milestone payment from EMD Serono in
November 2010 strengthened the Company’s cash position to a level comparable to that of year-end
2009. Finance costs in fiscal 2010 were a gain of $493,000 compared to an expense of $661,000 in
fiscal 2009. Finance costs in fiscal 2010 benefited from a net foreign currency gain of $511,000
compared to a net foreign currency loss of $635,000 in 2009.

Net Results

Reflecting the changes in revenue and expenses described above, we realized a net profit of
$8,930,000 ($0.15 per share) for the year ended November 30, 2010, compared to a net loss of
$15,156,000 ($0.25 loss per share) for the same period in fiscal 2009. The net profit included
revenue of $31,846,000 related to the collaboration and licensing agreement with EMD Serono.

- 7 - 

 

Quarterly Financial Information

The following table is a summary of the unaudited consolidated operating results of the Company
presented in accordance with IFRS for the last eight quarters.

(in thousands of Canadian dollars, except per share amounts)

	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	2010	 	 	 	 	 	 	 	 	 	 	 	 	 	2009
	 	 	Q4	 	Q3	 	Q2	 	Q1	 	Q4	 	Q3	 	Q2	 	Q1
	 
	Revenue
	 	$	26,717	 	 	$	1,717	 	 	$	1,717	 	 	$	1,717	 	 	$	1,718	 	 	$	12,601	 	 	$	1,717	 	 	$	1,432	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Net profit (net loss)
	 	$	21,299	 	 	$	(3,357	)	 	$	(4,771	)	 	$	(4,241	)	 	$	(4,654	)	 	$	5,779	 	 	$	(5,454	)	 	$	(10,827	)
	 
	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 	 
	Basic and diluted earnings
(loss) per share
	 	$	0.35	 	 	$	(0.06	)	 	$	(0.08	)	 	$	(0.07	)	 	$	(0.08	)	 	$	0.10	 	 	$	(0.09	)	 	$	(0.18	)

As described above, the higher revenue in the third quarter of 2009 is related to the milestone
payment of $10,884,000 received from EMD Serono following the FDA’s acceptance to file the
Company’s NDA for EGRIFTATM. The higher revenue in the fourth quarter of 2010 is related
to the receipt from EMD Serono of a milestone payment of $25,000,000 following marketing approval
of EGRIFTATM by the FDA.

Fourth Quarter Comparison

Consolidated revenue for the three-month period ended November 30, 2010, amounted to $26,717,000,
compared to $1,718,000 for the same period in fiscal 2009. The higher revenue in the three-month
period ended November 30, 2010 is related to the milestone payment of $25,000,000 received at the
end of the fourth quarter, following marketing approval of EGRIFTATM by the FDA in the
United States.

Consolidated R&D expenses, net of tax credits, totaled $3,172,000 for the fourth quarter of 2010,
compared to $4,212,000 for the same period in 2009, a decrease of 24.7%. The R&D expenses incurred
in 2009 principally included expenses related to preparing for the FDA Advisory Committee meeting,
which was held on May 27, 2010. The R&D expenses incurred in the fourth quarter of fiscal 2010 were
mainly related to managing responses to the FDA’s questions and the FDA approval process, in
addition to the advancement of our regulatory filing in Europe and on a new presentation of the
existing formulation of EGRIFTATM. Furthermore, we are in the process of evaluating the
initiation of a new clinical program to develop tesamorelin for a new indication. In our discovery
and preclinical groups, we continued to develop new peptides and to advance our preclinical program
in AKI.

General and administrative expenses were $2,036,000 in the fourth quarter of 2010, compared to
$1,563,000 for the same period in 2009. The higher expenses for 2010 are principally related to the
conversion of our financial statements to IFRS and FDA approval of EGRIFTATM in the
United States.

Selling and market development expenses amounted to $761,000 for the fourth quarter of 2010,
compared to $1,069,000 for the same period in 2009. The sales and market development

- 8 - 

 

expenses in fiscal 2010 are principally composed of business development expenses outside the
United States and the costs of performing our obligations under the agreement with EMD Serono. The
increased costs in 2009 were principally due to market development costs in Europe to increase the
awareness of lipodystrophy as a disease.

Consequently, we recorded a net profit for the three-month period ended November 30, 2010, of
$21,299,000 ($0.35 per share), compared to a net loss of $4,654,000 ($0.08 per share) for the same
period in 2009.

In the three-month period ended November 30, 2010, cash flows from operating activities, excluding
changes in operating assets and liabilities, was $22,037,000, compared to a use of cash of
$4,333,000 for the same period in 2009.

Liquidity and Capital Resources

Our objective in managing capital is to ensure a sufficient liquidity position to finance our
research and development activities, general and administrative expenses, working capital and
capital spending.

To fund our activities, we have relied primarily on public offerings of common shares in Canada and
private placements of our common shares as well as on up-front payments and milestone payments
primarily associated with the agreement with EMD Serono. When possible, we try to optimize our
liquidity position using non-dilutive sources, including investment tax credits, grants and
interest income.

For the year ended November 30, 2010, cash flow from operating activities, excluding changes in
operating assets and liabilities, was $11,160,000 compared to a use of cash of $13,547,000 in
fiscal 2009. The cash flow generated in fiscal 2010 is principally related to payments received
under the agreement with EMD Serono as well as decreases in R&D expenses and in selling and market
development expenses.

At November 30, 2010, cash and bonds amounted to $64,550,000 and tax credits and grants receivable
amounted to $332,000, for a total of $64,882,000.

At this time, apart from our unused $1,800,000 revolving credit facility, we do not have any
additional arrangements for external debt financings, and are not certain whether any proposed debt
financing in the future, would be available on acceptable terms, or available at all. We may seek
additional capital through the incurrence of debt, the issuance of equity or other financing
alternatives.

We invest our available cash in highly liquid fixed income instruments from governmental, municipal
and paragovernmental bodies ($37,542,000 at November 30, 2010) as well as corporate bonds with high
credit ratings ($359,000 at November 30, 2010).

In the year ended November 30, 2010, the Company received share subscriptions amounting to $15,000
($96,000 in fiscal 2009) for the issuance of 2,880 common shares (34,466 in 2009) in connection
with the share purchase plan. Under the terms of the agreement with EMD Serono, we issued 2,179,837 common shares for a cash consideration of
US$8,000,000 (C$9,854,000) during the first quarter of 2009.

- 9 -

 

In fiscal 2010, our third-party suppliers began to manufacture inventory of EGRIFTATM
for commercialization in the United States. We expect to continue to build our inventory
until we reach an adequate level of finished goods to meet the needs of our partners and this will
significantly increase our working capital needs in fiscal 2011.

Contractual Obligations

Commitments

We rent our headquarters and main office pursuant to a lease expiring in April 2021. At November
30, 2010 and 2009, and at December 1, 2008, the minimum payments required under the terms of the
non-cancellable lease were as follows:

	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	November 30,	 	 	November 30,	 	 	December 1,	 
	(in thousands of Canadian dollars)	 	2010	 	 	2009	 	 	2008	 
	 
	Less than one year
	 	 	55	 	 	 	340	 	 	 	816	 
	Between one and five years
	 	 	2,239	 	 	 	2,020	 	 	 	340	 
	More than five years
	 	 	3,943	 	 	 	4,216	 	 	 	—	 
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	 
	 
	 	 	6,237	 	 	 	6,576	 	 	 	1,156	 

Long-Term Procurement Agreements

During and after the years ended November 30, 2010 and 2009, we entered into long-term procurement
agreements with third-party suppliers in anticipation of the commercialization of
EGRIFTATM.

Credit Facility

We have a $1,800,000 revolving credit facility, bearing interest at prime plus 0.5%. Under the term
of the revolving credit facility, the market value of investments held must always be equivalent to
150% of amounts drawn under the facility. If the market value falls below $7,000,000, we will
provide the bank with a first rank movable hypothec (security interest) of $1,850,000 on securities
judged satisfactory by the bank. As at November 30, 2010, we did not have any borrowings
outstanding under this credit facility.

Post-Approval Commitments

In connection with its approval, the FDA has required the following three post-approval commitments:

	 	•	 	a single vial formulation of EGRIFTATM (the development of a new presentation of
the same formulation);
	 
	 	•	 	a long-term observational safety study using EGRIFTATM; and
	 
	 	•	 	a Phase 4 clinical trial using EGRIFTATM.

We have developed a new presentation of EGRIFTATM which is more user-friendly than its
current presentation because we expect it to be quicker and easier for a patient to manipulate. In
the new presentation of the same formulation, EGRIFTATM will be available as a single
unit dose (one vial containing 2 mg of tesamorelin) of sterile, lyophilized powder to be
reconstituted with

- 10 -

 

sterile water for injection. This new presentation complies with the first of the FDA’s
post-approval requirements. The FDA requires that this new presentation be available by November
2013.

The purpose of the long-term observational study required by the FDA is to evaluate the safety
of long-term administration of EGRIFTATM. The primary purpose of the Phase 4
clinical trial is to assess whether EGRIFTATM has an impact on diabetic retinopathy in
diabetic HIV-infected patients with lipodystrophy and excess abdominal fat. The FDA requires that
the proposals for the long-term observational safety study and Phase 4 clinical trial be completed
within six months of our having received approval to commercialize EGRIFTATM. Under the
terms of our collaboration and licensing agreement, EMD Serono is responsible for finalizing such
proposals. We will continue to support EMD Serono in developing and finalizing such proposals.

Contingent Liability

On July 26, 2010, we received a motion of authorization to institute a class action lawsuit against
the Company, a director and a former executive officer (the “Motion”). This Motion was filed in the
Superior Court of Quebec, district of Montreal. The applicant is seeking to initiate a class action
suit to represent the class of persons who were shareholders at May 21, 2010 and who sold their
common shares of the Company on May 25 or 26, 2010. This applicant alleges that the Company did not
comply with its continuous disclosure obligations as a reporting issuer by failing to disclose
certain alleged adverse effects relating to the administration of EGRIFTATM. The Company
is of the view that the allegations contained in the Motion are entirely without merit and intends
to take all appropriate actions to vigorously defend its position.

The Motion has not yet been heard by the Superior Court of Quebec and a date has not been set for
the hearing.

The Company has subscribed to insurance covering its potential liability and the potential
liability of its directors and officers in the performance of all their duties for the Company
subject to a $200,000 deductible. At November 30, 2010, an amount of $96,000 in legal fees had been
accrued and included in general and administrative expenses, of which $61,000 was paid during the
year and $35,000 remained in accounts payable and accrued liabilities.

Off-Balance Sheet Arrangements

We were not involved in any off-balance sheet arrangements for the year ended November 30,
2010, with the exception of the lease of our headquarters as described above.

Subsequent Events

Distribution and Licensing Agreements

On December 6, 2010, we announced the signing of a distribution and licensing agreement with Sanofi
covering the commercial rights for EGRIFTATM in Latin America, Africa, and the Middle East for the treatment of excess abdominal fat in HIV-infected patients with
lipodystrophy.

Under the terms of the Agreement, we will sell EGRIFTATM to Sanofi at a transfer price
equal to the higher of a percentage of Sanofi’s net selling price and a predetermined floor price.
We have retained all future development rights to EGRIFTATM and will be responsible for
conducting

- 11 -

 

research and development for any additional potential indications. Sanofi will be responsible for
conducting all regulatory activities for EGRIFTATM in the aforementioned territories,
including applications for approval in the different countries for the treatment of excess
abdominal fat in HIV-infected patients with lipodystrophy. We also granted Sanofi an option to
commercialize tesamorelin for other indications in the territories mentioned above. If such option
is not exercised, or is declined, by Sanofi, we may commercialize tesamorelin for such indications
on our own or with a third-party.

On February 3, 2011, we entered into a distribution and licensing agreement with Ferrer covering
the commercial rights for EGRIFTATM for the treatment of excess abdominal fat in
HIV-infected patients with lipodystrophy in Europe, Russia, South Korea, Taiwan, Thailand and
certain central Asian countries.

Under the terms of the Agreement, we will sell EGRIFTATM to Ferrer at a transfer price
equal to the higher of a significant percentage of Ferrer’s net selling price and a predetermined
floor price. We have retained all development rights to EGRIFTATM for other indications
and will be responsible for conducting research and development for any additional programs. Ferrer
will be responsible for conducting all regulatory and commercialization activities in connection
with EGRIFTATM for the treatment of excess abdominal fat in HIV-infected patients with
lipodystrophy in the territories subject to the agreement. We will be responsible for the
manufacture and supply of EGRIFTATM to Ferrer. We have the option to co-promote
EGRIFTATM for the reduction of excess abdominal fat in HIV-infected patients with
lipodystrophy in the territories. Ferrer has the option to enter into a co-development and
commercialization agreement using tesamorelin relating to any such new indications. The terms and
conditions of such a co-development and commercialization agreement will be negotiated based on any
additional program chosen for development.

Deferred Share Unit Plan

In December 2010, we adopted a deferred share unit plan (“Plan”) to provide long-term incentive
compensation for our directors and executive officers. Under the Plan, directors must receive their
annual remuneration as a board member in fully vested deferred share unites (“DSUs”) until they
reach a percentage of their annual remuneration and, once such percentage is attained, they have
the option to elect to receive part or all of their annual remuneration in DSUs. Under the plan,
executive officers have the option of receiving all or a portion of their annual bonus in the form
of fully-vested DSUs. The units are only redeemable for cash when a participant ceases to be an
employee or member of the Board of Directors. We manage the risk associated with the issuance of
the DSU by entering into a yearly forward contract with a third-party. As at February 7,
2011, all of the 99,912 DSUs outstanding were covered by a prepaid forward contract.

Stock Option Plan

Between December 1, 2010 and February 7, 2011, the Company granted 250,000 options at an exercise
price of $5.65 per share. Also, 27,832 options were forfeited and expired at a weighted exercise
average price of $12.06 per share and 3,000 options were exercised at a weighted exercise average
price of $1.80 per share for a cash consideration of $5,000.

- 12 -

 

Financial Risk Management

This section provides disclosure relating to the nature and extent of our exposure to risks
arising from financial instruments, including credit risk, liquidity risk, currency risk and
interest rate risk, and how we manage those risks.

Credit Risk

The Company’s exposure to credit risk currently relates to accounts receivables with only one
customer (see note 4 of the Audited Consolidated Financial Statements). Credit risk is the risk of
an unexpected loss if a customer or counterparty to a financial instrument fails to meet its
contractual obligations. We regularly monitor credit risk exposure and take steps to mitigate the
likelihood of this exposure resulting in losses.

Financial instruments other than cash and trade and other receivables that potentially subject the
Company to significant credit risk consist principally of bonds. We invest our available cash in
highly liquid fixed income instruments from governmental, paragovernmental and municipal bodies
($37,542,000 as at November 30, 2010) as well as from companies with high credit ratings ($359,000
as at November 30, 2010). As at November 30, 2010, we were not exposed to any credit risk over the
carrying amount of the bonds.

Liquidity Risk

Liquidity risk is the risk that we will not be able to meet our financial obligations as they
become due. We manage liquidity risk through the management of our capital structure, as outlined
under “Liquidity and Capital Resources”. We also manage liquidity risk by continuously monitoring
actual and projected cash flows. The Board of Directors and/or the Audit Committee reviews and
approves our operating and capital budgets, as well as any material transactions out of the
ordinary course of business.

We have adopted an investment policy in respect of the safety and preservation of capital to ensure
that our liquidity needs are met. The instruments are selected with regard to the expected timing
of expenditures and prevailing interest rates.

The required payments on the contractual maturities of financial liabilities, as well as the
payments required under the terms of the operating lease, as at November 30, 2010, are presented in
notes 20 and 23 of the Audited Consolidated Financial Statements.

Currency Risk

We are exposed to financial risk related to the fluctuation of foreign exchange rates and the
degree of volatility of those rates. Currency risk is limited to the portion of our business
transactions denominated in currencies other than the Canadian dollar, primarily revenues from
milestone payments and expenses for research and development incurred in U.S. dollars, euros and
pounds sterling (“GBP”). We do not use derivative financial instruments to reduce our foreign
exchange exposure.

We manage currency risk by maintaining cash in U.S. dollars on hand to support U.S. forecasted cash
budgets for a maximum 12-month period. We do not currently view our exposure to the euro and GBP as a significant foreign exchange risk due to the limited volume of
transactions conducted by the Company in these currencies.

Exchange rate fluctuations for foreign currency transactions can cause cash flow as well as amounts
recorded in consolidated statement of comprehensive income to vary from period to

- 13 -

 

period and not necessarily correspond to those forecasted in operating budgets and projections.
Additional earnings variability arises from the translation of monetary assets and liabilities
denominated in currencies other than the Canadian dollar at the rates of exchange at each
consolidated statement of financial position date, the impact of which is reported as foreign
exchange gain or loss in the consolidated statement of comprehensive income. Given our policy on
the management of our U.S. foreign currency risk, we do not believe, a sudden change in foreign
exchange rates would impair or enhance our ability to pay our U.S. dollar denominated obligations.

The following table provides significant items exposed to currency risk as at November 30, 2010:

	 	 	 	 	 	 	 	 	 	 	 	 	 
	 	 	 	 	 	 	 	 	 	 	November 30,	 
	 	 	 	 	 	 	 	 	 	 	2010	 
	(in thousands of dollars)	 	$US	 	 	EURO	 	 	GBP	 
	 
	Cash
	 	 	26,424	 	 	 	—	 	 	 	1	 
	Trade and other receivables
	 	 	—	 	 	 	—	 	 	 	—	 
	Accounts payable and accrued liabilities
	 	 	(465	)	 	 	(26	)	 	 	(81	)
	 
	 	 	 	 	 	 	 	 	 	 	 	 
	 
	Items exposed to currency risk
	 	 	25,959	 	 	 	(26	)	 	 	(80	)

The following exchange rates applied during the year ended November 30, 2010:

	 	 	 	 	 	 	 	 	 
	 	 	Average rate	 	Reporting date rate
	 

	$US — C$
	 		1.0345	 	 	 	1.0266	 
	EURO — C$
	 		1.3848	 	 	 	1.3326	 
	GBP — C$
	 		1.6051	 	 	 	1.5969	 
	 

In fiscal 2010, based on our foreign currency exposures noted above, varying the above foreign
exchange rates to reflect a 5% strengthening of the Canadian dollar would have increased the net
profit as follows, assuming that all other variables remained constant:

	 	 	 	 	 	 	 	 	 	 	 	 	 
	(in thousands of dollars)	 	$US	 	EURO	 	GBP
	 
	Increase in net profit
	 	 	1,298	 	 	 	(1	)	 	 	(4	)
	 

An assumed 5% weakening of the Canadian dollar would have had an equal but opposite effect on
the above currencies to the amounts shown above, assuming that all other variables remain constant.

Interest Rate Risk

Interest rate risk is the risk that the fair value or future cash flows of a financial instrument
will fluctuate because of changes in market interest rates.

Our short-term bonds are invested at fixed interest rates and/or mature in the short-term.
Long-term bonds are also instruments that bear interest at fixed rates. The risk that we will
realize a

- 14 -

 

loss as a result of a decline in the fair value of our bonds is limited because these
investments, although they are classified as available for sale, are generally held to maturity.
The unrealized gains or losses on bonds are recorded in accumulated other comprehensive income.

Based on the value of our short and long-term bonds at November 30, 2010, an assumed 0.5% decrease
in market interest rates would have increased the fair value of these bonds and the accumulated
other comprehensive income by approximately $336,000; an assumed increase in interest rate of 0.5%
would have an equal but opposite effect, assuming that all other variables remained constant.

Cash bears interest at a variable rate. Trade and other receivables, accounts payable and accrued
liabilities bear no interest.

Based on the average value of variable interest-bearing cash during year ended November 30, 2010
($3,219,000), an assumed 0.5% increase in interest rates during such period would have increased
the future cash flow and the net profit by approximately $16,000; an assumed decrease of 0.5% would
have had an equal but opposite effect.

Financial Instruments

We have determined that the carrying values of our short-term financial assets and
liabilities, including cash, trade and other receivables as well as accounts payable and accrued
liabilities, approximate their fair value because of the relatively short period to maturity of the
instruments. 

Bonds are stated at estimated fair value, determined by inputs that are primarily
based on broker quotes at the reporting date (level 2 inputs — see note 22 — Determination of
fair values).

Critical Accounting Estimates

Use of Estimates and the Exercise of Judgment

The preparation of our Audited Consolidated Financial Statements in conformity with IFRS requires
management to make estimates and assumptions that affect the reported amounts of assets and
liabilities and disclosure of contingent assets and liabilities at the date of the financial
statements and the reported amounts of revenues and expenses during the reporting period.

Information about critical judgments in applying accounting policies and assumption and estimation
uncertainties that have the most significant effect on the amounts recognized in the consolidated
financial statements is included in the following notes to the Audited Consolidated Financial
Statements:

Note 4 — Revenue and deferred revenue

Note 15 (iv) — Stock option plan

Note 16 — Income taxes

Note 18 — Contingent liability

Other areas of judgement and uncertainty relate to the estimation of accruals for clinical trial
expenses, the recoverability of inventories, the measurement of the amount and assessment of the
recoverability of tax credits and grants receivable and capitalization of development expenditures.

- 15 -

 

Reported amounts and note disclosure reflect the overall economic conditions that are most likely
to occur and the anticipated measures management intends to take. Actual results could differ from
those estimates.

The above estimates and assumptions are reviewed regularly. Revisions to accounting estimates are
recognized in the period in which the estimates are revised and in any future periods affected.

Conversion to IFRS

In February 2008, the Accounting Standards Board of Canada (“AcSB”) announced that accounting
standards in Canada, as used by public companies, would converge with IFRS, for financial periods
beginning on and after January 1, 2011 with the option to early adopt IFRS upon receipt of approval
from the Canadian Securities regulatory authorities. In the fourth quarter, we filed a request to
adopt IFRS two years in advance of the date required under the AcSB, using December 1, 2008 as the
date of transition and December 1, 2009 as the changeover date. Our request was granted and as a
result, the consolidated financial statements for the year ended November 30, 2010 are our first
annual financial statements prepared in conformity with IFRS.

Because we had previously filed financial statements and MD&As for the first, second and third
quarters of 2010 with comparisons to 2009 in accordance with Canadian GAAP, these statements were
restated and re-filed on February 8, 2011 to reflect our adoption of IFRS. Periods prior to
December 1, 2008 have not been restated.

In preparing these first IFRS financial statements, we used the IFRS accounting policies in effect
as at November 30, 2010, including IFRS 1 — First-time Adoption of International Financial
Reporting Standards (“IFRS 1”). IFRS 1 provides guidance for an entity’s initial adoption of IFRS
and outlines that, in general, an entity applies the principles under IFRS retrospectively with
adjustments arising on conversion from Canadian GAAP to IFRS being directly recognized in retained
earnings as of the beginning of the first comparative financial statements presented. IFRS 1 also
requires companies adopting IFRS to reconcile equity and net earnings from the previously reported
Canadian GAAP amounts to the restated IFRS amounts. Our reconciliation of equity under Canadian
GAAP as at December 1, 2008, the date of transition, and as at November 30, 2009 to the restated
IFRS amounts are included in note 27 of the consolidated financial statements, as is the
reconciliation of comprehensive income for the year-ended November 30, 2009.

IFRS 1 also provides certain optional exemptions from retrospective application of certain IFRS
requirements as well as mandatory exceptions which prohibit retrospective application of standards.

We elected to apply the following optional exemptions from full retrospective application:

(i) IFRS 2 — Share-based Payment: IFRS 1 encourages the application of IFRS 2, Share-based
Payment provisions to equity instruments granted on or before November 7, 2002, but permits
the application only to equity instruments granted after November 7, 2002 that were not
vested by the transition date. As permitted by this exemption, the Company applied IFRS 2
only to equity instruments granted after November 7, 2002 that were not vested by December
1, 2008.

(ii) Designation of financial assets and financial liabilities exemption: we elected to
redesignate cash from the held for trading category to loans and receivables.

- 16 -

 

We also followed the mandatory exemptions applicable to the Company as described below:

Estimates — Hindsight cannot be used to create or revise estimates. Estimates previously
made under Canadian GAAP cannot be revised for application of IFRS except where necessary
to reflect any difference in accounting policies.

Impact of IFRS on the Company’s Financial Statements

The adoption of IFRS resulted in some changes to our accounting policies that were applied in the
recognition, measurement and disclosure of balances and transactions in our financial statements.
However, none of the changes to our accounting policies resulted in significant changes to line
items within our financial statements.

The following provides a summary of our evaluation of important changes to accounting policies in
key areas:

IFRS 2, Share-based Payment (“IFRS 2”)

Under IFRS, when stock option awards vest gradually, each tranche is to be considered as a separate
award, while under Canadian GAAP, companies can make a policy choice to consider gradually vested
tranches as a single award. Similarly, the IFRS standard requires that forfeiture estimates be
established at the time of the initial fair value assessment of share-based payments rather than to
account for the forfeitures as they occur. Therefore, the compensation expense will have to be
recognized over the expected term of each tranche and take into account the impact of the
differences in accounting for forfeitures. As a result of this change, an amount of $175,000 was
recorded to deficit at the transition date, with the counterpart to contributed surplus.

IAS 36, Impairment of Assets (“IAS 36”)

Under Canadian GAAP impairment standards for non-financial assets, a write-down to estimated fair
value is recognized if the estimated undiscounted future cash flows from an asset or group of
assets are less than their carrying value. IAS 36 requires a write-down to be recognized if the
recoverable amount, determined as the higher of the estimated fair value less costs to sell or
value in use, is less than carrying value. We performed impairment testing as of December 1, 2008
and concluded that no impairment charge was required under IFRS. No impairment indicators were
identified for the period between the transition date and November 30, 2009 and November 30, 2010.
IAS 36 also permits the reversal of certain impairment charges where conditions have changed. We
reviewed past impairment charges and concluded that there was no justification for reversal of past
impairment charges.

IAS 1, Presentation of Financial Statements (“IAS 1”)

Financial statement presentation is addressed in conjunction with the related IFRS standards.
Certain additional disclosures were required in the notes to the financial statements and the
statement of comprehensive income was modified to reflect a presentation by function. The
reclassifications required as a result of this change are described in note 27 (c) of the
consolidated financial statements.

Other Standards

Our examination of all other standards, including for example, IAS 21 — The Effects of Changes in
Foreign Exchange Rates, IAS 37 — Provisions, Contingent Liabilities and Contingent Assets, and IAS
18 — Revenue, revealed no significant adjustment was necessary other than enhanced disclosures.

- 17 -

 

Note 27 of the consolidated financial statements for the year ended November 30, 2010 contains a
detailed description of our conversion to IFRS, including a line-by-line reconciliation of our
financial statements previously prepared under Canadian GAAP to those under IFRS as at November 30,
2009 and December 1, 2008.

Impact on the Business

The impact of the conversion to IFRS on the Company was minimal and therefore resulted in a limited
number of adjustments. Our systems easily accommodated the required changes. Our internal controls
and disclosure controls and procedures did not require significant modification as a result of its
conversion to IFRS. Furthermore, there was no impact on our contractual arrangements or compliance
thereto.

Impact on Information Systems and Technology

The transition had minimal impacts on our information systems. The areas where information systems
were most impacted were minor modifications to certain general ledger accounts, sub-ledgers and
end-user reports to accommodate IFRS accounting adjustments, recording, and heightened disclosures.

Impact on Internal Control over Financial Reporting and Disclosure Controls and Procedures

Our internal controls over financial reporting were also not significantly affected by the
transition to IFRS. The IFRS differences required presentation and process changes to report more
detailed information in the notes to the financial statements, as well as certain changes to the
recognition and measurement practices. Disclosure controls and procedures were adapted to take into
consideration the changes in recognition, measurement and disclosure practices but the impact was
minimal as well.

Impact on Financial Reporting Expertise

Training and education was provided to all members of the finance team who are directly affected by
the transition to IFRS. This training focused mainly on the process changes required and an
overview of the reasons behind the changes from a standards perspective.

New accounting policies

Certain pronouncements were issued by the IASB or International Financial Reporting
Interpretation Committee that are mandatory for annual periods beginning after January 1, 2010 or
later periods. Many of these updates are not applicable or are inconsequential to us and have been
excluded from the discussion below. The remaining pronouncements are being assessed to determine
their impact on our results and financial position:

Annual improvements to IFRS

The IASB’s improvements to IFRS published in April 2009 contain fifteen amendments to twelve
standards that result in accounting changes for presentation, recognition or
measurement purposes largely for annual periods beginning on or after January 1, 2010, with early
adoption permitted. These amendments were considered by the Company and deemed to be not applicable
to the Company other than for the amendment to IAS 17 — Leases relating to leases which include
both land and buildings elements. In this case, the Company early adopted this amendment.

- 18 -

 

The IASB’s improvements to IFRS contain seven amendments that result in accounting changes for
presentation, recognition or measurement purposes. The most significant features of the IASB’s
annual improvements project published in May 2010 are included under the specific revisions to
standards discussed below.

	(i)	 	IFRS 3:
	 
	 	 	Revision to IFRS 3, Business Combinations:

	 	 	 	Effective for annual periods beginning on or after July 1, 2010 with earlier adoption
permitted.
	 
	 	 	 	Clarification on the following areas:

	 	•	 	the choice of measuring non-controlling interests at fair value or at the
proportionate share of the acquiree’s net assets applies only to instruments that
represent present ownership interests and entitle their holders to a proportionate
share of the net assets in the event of liquidation. All other components of
non-controlling interest are measured at fair value unless another measurement basis is
required by IFRS.
	 
	 	•	 	application guidance relating to the accounting for share-based payments in IFRS
3 applies to all share-based payment transactions that are part of a business
combination, including un-replaced awards (i.e., unexpired awards over the acquiree shares that remain outstanding rather than being replaced by the acquirer) and
voluntarily replaced share-based payment awards.

	(ii)	 	IFRS 7:

	 	 	 	Amendment to IFRS 7, Financial Instruments: Disclosures:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2011 with earlier
adoption permitted.
	 
	 	 	 	Multiple clarifications related to the disclosure of financial instruments and in
particular in regards to transfers of financial assets.

	(iii)	 	IAS 1:

	 	 	 	Amendment to IAS 1, Presentation of Financial Statements:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2011 with earlier
adoption permitted.
	 
	 	 	 	Entities may present the analysis of the components of other comprehensive income
either in the statement of changes in equity or within the notes to the financial
statements.

	(iv)	 	IAS 27:

	 	 	 	Amendment to IAS 27, Consolidated and Separate Financial Statements:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2011 with earlier
adoption permitted.
	 
	 	 	 	The 2008 revisions to this standard resulted in consequential amendments to IAS 21,
The Effects of Changes in Foreign Exchange Rates, IAS 28, Investments in Associates,
and IAS 31, Interests in Joint Ventures. IAS 27 now provides that these amendments are
to be applied prospectively.

	(v)	 	IAS 34:

	 	 	 	Amendment to IAS 34, Interim Financial Reporting:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2011 with earlier
adoption permitted.
	 
	 	 	 	The amendments place greater emphasis on the disclosure principles for interim
financial reporting involving significant events and transactions, including changes to

- 19 -

 

	 	 	 	fair value measurements and the need to update relevant information from the most
recent annual report.

New or revised standards and interpretations

In addition, the following new or revised standards and interpretations have been issued but are
not yet applicable to the Company:

	(i)	 	IAS 24:

	 	 	 	Amendments to IAS 24, Related Party Disclosures:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2011 with earlier
adoption is permitted.
	 
	 	 	 	There are limited differences in the definition of what constitutes a related party;
however, the amendment requires more detailed disclosures regarding commitments.
	 
	 	(ii)	 	IFRS 8:
	 
	 	 	 	IFRS 8, Operating Segments:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2010.
	 
	 	 	 	Requires purchase information about segment assets.

	(iii)	 	IFRS 9:

	 	 	 	New standard IFRS 9, Financial Instruments:
	 
	 	 	 	Effective for annual periods beginning on or after January 1, 2013 with earlier
adoption permitted.
	 
	 	 	 	As part of the project to replace IAS 39, Financial Instruments: Recognition and
Measurement, this standard retains but simplifies the mixed measurement model and
establishes two primary measurement categories for financial assets. More specifically,
the standard:

	 	•	 	deals with classification and measurement of financial
assets
	 
	 	•	 	establishes two primary measurement categories for financial assets:
amortized cost and fair value
	 
	 	•	 	classification depends on entity’s business
model and the contractual cash flow characteristics of the financial asset
	 
	 	•	 	eliminates the existing categories: held to maturity, available for sale, and
loans and receivables.

Certain changes were also made regarding the fair value option for financial liabilities and
accounting for certain derivatives linked to unquoted equity instruments.

Outstanding share data

At February 7, 2011, the common shares issued and outstanding were 60,515,764 while
outstanding options granted under the stock option plan were 3,068,306.

- 20 -

 

Disclosure controls and procedures and internal control over financial reporting

As at November 30, 2010, an evaluation of the design and operating effectiveness of our
disclosure controls and procedures, as defined in the rules of Canadian Securities Administrators,
was carried out. Based on that evaluation, the President and Chief Executive Officer and the Senior
Executive Vice-President and Chief Financial Officer concluded that the design and operating
effectiveness of those disclosure controls and procedures were effective.

Also as November 30, 2010, an evaluation of the design and operating effectiveness of internal
controls over financial reporting, as defined in the rules of the Canadian Securities
Administrators, was carried out to provide reasonable assurance regarding the reliability of
financial reporting and financial statement compliance with IFRS. Based on that evaluation, the
President and Chief Executive Officer and the Senior Executive Vice-President and Chief Financial
Officer concluded that the design and operating effectiveness of internal controls over financial
reporting were effective.

These evaluations were based on the framework established in Internal Control —Integrated
Framework issued by the Committee of Sponsoring Organizations of the Treadway Commission, a
recognized control model, and the requirements of Multilateral Instrument 52-109 of the Canadian
Securities Administrators. A disclosure committee comprised of members of senior management assists
the President and Chief Executive Officer and the Senior Executive Vice-President and Chief
Financial Officer in their responsibilities.

All control systems, no matter how well designed, have inherent limitations, including the
possibility of human error and the circumvention or overriding of the controls or procedures. As a
result, there is no certainty that our disclosure controls and procedures or internal control over
financial reporting will prevent all errors or all fraud. There were no changes in our internal
controls over financial reporting that occurred during the year ended November 30, 2010 that have
materially affected, or are reasonably likely to materially affect, our internal controls over
financial reporting.

Risks and uncertainties

Investors should understand that we operate in a high risk industry. We have identified the
following risks and uncertainties that may have a material adverse effect on our business,
financial condition or operating results. Investors should carefully consider the risks described
below before purchasing our securities. The risks described below are not the only ones that we
face. Additional risks not presently known to us or that we currently believe are immaterial may
also significantly impair our business operations. Our business could be harmed by any of these
risks.

- 21 -

 

Risks Related to the Commercialization of our Product and Product Candidates

Our commercial success depends largely on the commercialization of EGRIFTATM; the
failure of EGRIFTATM to obtain commercial acceptance would have a material adverse
effect on us.

Our ability to generate revenues in the future is primarily based on the commercialization of
EGRIFTATM for the reduction of excess abdominal fat in HIV-infected patients with
lipodystrophy. In the short-term, these revenues should be primarily derived from the U.S. market
alone. Although we have entered into a collaboration and licensing agreement with EMD Serono for
the commercialization of EGRIFTATM in the United States, there can be no assurance that
EGRIFTATM will be successfully commercialized in the United States, or in any other
country. Although we are developing other peptides, all of them are at earlier stages of
development and none of them may reach the clinical trial phase, obtain regulatory approval or,
even if approved, be successfully commercialized.

The overall commercialization success of EGRIFTATM for the reduction of excess abdominal
fat in HIV-infected patients with lipodystrophy will depend on several factors, including:

	 	•	 	receipt of regulatory approvals for EGRIFTATM from
regulatory agencies in the territories other than the United States in which we
wish to expand the commercialization of tesamorelin;
	 
	 	•	 	market acceptance of EGRIFTATM by the medical community,
patients and third-party payors (such as governmental health administration
authorities and private health coverage insurers);
	 
	 	•	 	the amount of resources devoted by our commercial partners to
commercialize EGRIFTATM in their respective territories;
	 
	 	•	 	maintaining manufacturing and supply agreements to ensure the
availability of commercial quantities of EGRIFTATM through validated
processes;
	 
	 	•	 	the number of competitors in our market; and
	 
	 	•	 	protecting and enforcing our intellectual property and avoiding patent
infringement claims.

The inability to commercialize EGRIFTATM in the United States for the reduction of
excess abdominal fat in HIV-infected patients with lipodystrophy in the short term would delay our
capacity to generate revenues and would have a material adverse effect on our financial condition
and operating results.

- 22 -

 

We are or will be dependent on a limited number of collaboration and licensing agreements for the
commercialization of EGRIFTATM in the United States, Europe, Latin America, Africa and
the Middle East. These agreements place the commercialization of EGRIFTATM in these
markets outside of our control.

Although our collaboration and licensing agreements with EMD Serono, Sanofi and Ferrer contain
provisions governing their respective responsibilities as partners for the commercialization of
EGRIFTATM in their respective territories, our dependence on these partners to
commercialize EGRIFTATM is subject to a number of risks, including:

	 	•	 	our limited control of the amount and timing of resources that our
commercial partners will be devoting to the commercialization, marketing and
distribution of tesamorelin, including obtaining patient reimbursement for
EGRIFTATM, which could adversely affect our ability to obtain or
maximize our royalty payments;
	 
	 	•	 	disputes or litigation that may arise between us and our commercial
partners, which could adversely affect the commercialization of tesamorelin, all
of which would divert our management’s attention and our resources;
	 
	 	•	 	our commercial partners not properly defending our intellectual
property rights or using them in such a way as to expose us to potential
litigation, which could, in both cases, adversely affect the value of our
intellectual property rights; and
	 
	 	•	 	corporate reorganizations or changes in business strategies of our
commercial partners, which could adversely affect a commercial partner’s
willingness or ability to fulfill its obligations under its respective agreement.

Our collaboration and licensing agreements may be terminated by our partners in the event of a
breach by us of our obligations under such agreements, including our obligation to supply
EGRIFTATM , for which we rely on third parties. Our collaboration and licensing
agreement with EMD Serono can also be terminated by EMD Serono for their convenience on 180 days
notice to us. Such a termination could have an adverse effect on our revenues related to the
commercialization of EGRIFTATM in the United States. In addition, EMD Serono has listed
a patent held by one of its affiliates in the Orange Book under the Hatch-Waxman Act with respect
to EGRIFTATM in HIV-associated lipodystrophy. In the event of a termination of our
agreement with EMD Serono, EMD Serono could assert that such patent would be infringed by our
continued sale of EGRIFTATM in the United States. Any such assertion would divert our
management’s attention and could have a material adverse effect on our results of operations.

If any one of our commercial partners terminates their agreement with us or fails to effectively
commercialize EGRIFTATM, for any of the foregoing or other reasons, we may not be able
to replace the commercial partner and any of these events would have a material adverse effect on
our business, results of operations and our ability to achieve future profitability, and could
cause our stock price to decline.

We rely on third parties for the manufacture and supply of EGRIFTATM and tesamorelin and
such reliance may adversely affect us if the third parties are unable or unwilling to fulfill their
obligations.

The manufacture of pharmaceutical products requires significant expertise and capital investment,
including the development of advanced manufacturing techniques and process

- 23 -

 

controls. We do not own or operate manufacturing facilities for the production of tesamorelin or
any of our other product candidates, nor do we have plans to develop our own manufacturing
operations in the foreseeable future. We currently rely on third parties to manufacture and supply
all of our required raw materials, drug substance and drug product for our preclinical research,
clinical trials and commercial sales. For tesamorelin for clinical studies and EGRIFTATM
for commercial sales, we are currently using, and relying on, single suppliers and single
manufacturers for starting materials and the final drug substance. Although potential alternative
suppliers and manufacturers have been identified, we have not qualified these vendors to date and
no assurance can be given that such suppliers will be qualified in the future or receive necessary
regulatory approval.

Our reliance on third-party manufacturers exposes us to a number of risks. We may be subject to
delays in or suspension of the manufacturing of EGRIFTATM and tesamorelin if a
third-party manufacturer:

	 	•	 	becomes unavailable to us for any reason, including as a result of the
failure to comply with good manufacturing practices, or GMP, regulations;
	 
	 	•	 	experiences manufacturing problems or other operational failures, such
as equipment failures or unplanned facility shutdowns required to comply with GMP
or damage from any event, including fire, flood, earthquake, business
restructuring or insolvency; or
	 
	 	•	 	fails to perform its contractual obligations under our agreement, such
as failing to deliver the quantities requested on a timely basis.

Any delay in or suspension of the supply of EGRIFTATM could delay or prevent the sale of
EGRIFTATM and, accordingly, adversely affect our revenues and results of operations. In
addition, any manufacturing delay or delay in delivering EGRIFTATM may result in our
being in default under our collaboration agreements. If the damage to a supplier’s manufacturer
facility is extensive, or, for any reason, it does not operate in compliance with GMP or the
third-party manufacturer is unable or refuses to perform its obligations under our agreement, we
would need to find an alternative third-party manufacturer. The selection of a replacement
third-party manufacturer would be time-consuming and costly since we would need to validate the
manufacturing facility of such new third-party manufacturer. The validation process would include
an assessment of the capacity of such third-party manufacturer to produce the quantities that we
may request from time to time, the manufacturing process and its compliance with GMP. In addition,
the third-party manufacturer would have to familiarize itself with our technology. Any delay in
finding an alternative third-party manufacturer of tesamorelin and EGRIFTATM could
result in a shortage of such analogue or product, which could materially adversely affect our
business and results of operations.

Even though we have received regulatory approval for EGRIFTATM in the United States, we
still may not be able to successfully commercialize it if we do not gain market acceptance and the
revenue that we generate from its sales, if any, may be limited.

The commercial success of EGRIFTATM or any future products for which we obtain
marketing approval from the FDA or other regulatory authorities, will depend upon the acceptance
of such product by the medical community, including physicians, patients and health care payors.
The degree of market acceptance of any of our products will depend on a number of factors,
including:

- 24 -

 

	 	•	 	acceptance of the product by physicians and patients as safe and effective
treatments and addressing a significant unmet medical need;
	 
	 	•	 	product price;
	 
	 	•	 	the effectiveness of our sales and marketing efforts (or those of our
commercial partners);
	 
	 	•	 	storage requirements and ease of administration;
	 
	 	•	 	dosing regimen;
	 
	 	•	 	safety and efficacy;
	 
	 	•	 	prevalence and severity of side effects;
	 
	 	•	 	competitive products;
	 
	 	•	 	the ability to obtain and maintain sufficient third-party coverage or
reimbursement from government health care programs, including Medicare and
Medicaid, private health insurers and other third-party payors; and
	 
	 	•	 	the willingness and ability of patients to pay out-of-pocket in the
absence of third-party coverage.

If EGRIFTATM does not achieve an adequate level of acceptance by physicians, health care
payors and patients, we may not generate sufficient revenue from this product, and we may not be
able to achieve profitability. Our efforts, and the efforts of our commercial partners, to educate
the medical community and third-party payors on the benefits of tesamorelin may require significant
resources and may never be successful.

We have no internal sales, marketing or distribution capabilities so we must rely on strategic
alliance agreements with third parties for the sale and marketing of EGRIFTATM or any
future products.

We currently have no internal sales, marketing or distribution capabilities and we rely on our
commercial partners to market and sell EGRIFTATM in their respective territories. Our
agreements with our commercial partners contain termination provisions which, if exercised, could
delay or suspend the commercialization of EGRIFTATM or any future products.

In the event of any such termination, in order to continue commercialization, we would be required
to build our own sales force or enter into agreements with third parties to provide such
capabilities. We currently have limited marketing capabilities and we have limited experience in
developing, training or managing a sales force. The development of a sales force would be costly
and would be time-consuming given the limited experience we have in this area. To the extent we
develop a sales force, we could be competing against companies that have more experience in
managing a sales force than we have and that have access to more funds than we with which to manage
a sales force. Consequently, there can be no assurance that a sales force which we develop would be
efficient and would maximize the revenues derived from the sale of EGRIFTATM or any
future products.

- 25 -

 

We are substantially dependent on revenues from EGRIFTATM.

Our current and future revenues depend substantially upon sales of EGRIFTATM by our
commercial partners, EMD Serono, Sanofi and Ferrer. Any negative developments relating to this
product, such as safety or efficacy issues, the introduction or greater acceptance of competing
products, including those marketed and sold by our commercial partners, or adverse regulatory or
legislative developments, would have a material adverse effect on our business, prospects and
results of operations. Although we continue to develop additional product candidates for
commercialization, we expect to be substantially dependent on sales from EGRIFTATM for
the foreseeable future. A decline in sales from this product would adversely affect our business.

Our levels of revenues are highly dependent on obtaining patient reimbursement for
EGRIFTATM.

Market acceptance and sales of EGRIFTATM will substantially depend on the availability
of reimbursement from third party payors such as governmental authorities, including U.S. Medicare
and Medicaid, managed care providers, and private insurance plans and may be affected by healthcare
reform measures in the United States and elsewhere. Government authorities and third-party payors,
such as private health insurers and health maintenance organizations, decide which medications they
will pay for and establish reimbursement levels. A primary trend in the U.S. healthcare industry
and elsewhere is cost containment. Government authorities and these third-party payors have
attempted to control costs by limiting coverage and the amount of reimbursement for particular
medications. Increasingly, third-party payors have been challenging the prices charged for
products.

Under our agreements with our commercial partners, they are responsible for seeking reimbursement
of EGRIFTATM in their respective territories and as a result we have no control over
whether or what level of reimbursement is achieved.

We cannot be sure that reimbursement by insurers, government or other third parties will be
available for EGRIFTATM and, if reimbursement is available, the level of reimbursement
provided to patients. Reimbursement may impact the demand for, or the price of,
EGRIFTATM and our future products for which we obtain marketing approval. If
reimbursement is not available or is available only in limited amount, our commercial partners may
not be able to successfully commercialize EGRIFTATM or our future products and it will
have a material adverse effect on our revenues and royalties, business and prospects.

A variety of risks associated with our international business relationships could materially
adversely affect our business.

International business relationships in the United States, Europe, Latin America, Africa, the
Middle East and elsewhere subject us to additional risks, including:

	 	•	 	differing regulatory requirements for drug approvals in foreign countries;
	 
	 	•	 	potentially reduced protection for intellectual property rights;
	 
	 	•	 	potential third-party patent rights in foreign countries;

- 26 -

 

	 	•	 	the potential for so-called parallel importing, which is what happens when a local
seller, faced with high or higher local prices, opts to import goods from a foreign
market, with low or lower prices, rather than buying them locally;
	 
	 	•	 	unexpected changes in tariffs, trade barriers and regulatory requirements;
	 
	 	•	 	economic weakness, including inflation, or political instability,
particularly in foreign economies and markets;
	 
	 	•	 	compliance with tax, employment, immigration and labor laws for
employees traveling abroad;
	 
	 	•	 	foreign taxes;
	 
	 	•	 	foreign exchange contracts and foreign currency fluctuations, which
could result in increased operating expenses and reduced revenue, and other
obligations incident to doing business in another country;
	 
	 	•	 	workforce uncertainty in countries where labor unrest is more common
than in the United States and Canada;
	 
	 	•	 	production shortages resulting from any events affecting raw material
supply or manufacturing capabilities abroad; and
	 
	 	•	 	business interruptions resulting from geo-political actions, including
war and terrorism, or natural disasters, including earthquakes, volcanoes,
typhoons, floods, hurricanes and fires.

These and other risks of international business relationships may materially adversely affect our
business, prospects, results of operations and financial condition.

Governments outside the United States tend to impose strict price controls, which may adversely
affect our revenues, if any.

In several countries, including countries which are in Europe, Latin America, Africa, and the
Middle East, the pricing of prescription drugs may be subject to governmental control. In these
countries, pricing negotiations with governmental authorities can take considerable time and delay
the marketing of a product. To obtain reimbursement or pricing approval in some countries, a
clinical trial that compares the cost-effectiveness of a product candidate to other available
therapies may be required. If reimbursement of our product is unavailable or limited in scope or
amount, or if pricing is set at unsatisfactory levels, our commercial partners may not be willing
to devote resources to market and commercialize EGRIFTATM or may decide to cease
marketing such product. In such case, our business, prospects and results of operations could be
materially adversely affected.

We face competition and the development of new products by other companies could materially
adversely affect our business and products.

The biopharmaceutical and pharmaceutical industries are highly competitive and we must compete with
pharmaceutical companies, biotechnology companies, academic and research institutions as well as
governmental agencies for the development and commercialization of

- 27 -

 

products, most of which have substantially greater financial, technical and personnel resources
than us. Although we believe that we have no direct competitors for the reduction of excess
abdominal fat in HIV-infected patients with lipodystrophy, we could face indirect competition from
other companies developing and/or commercializing metabolic products and/or other products that
reduce or eliminate the occurrence of lipodystrophy.

In the other clinical programs that we are currently evaluating for development, there may exist
companies that are at a more advanced stage of developing a product to treat the diseases for which
we are evaluating clinical programs. Some of these competitors could have access to capital
resources, research and development personnel and facilities that are superior to ours. In
addition, some of these competitors could be more experienced than we are in the development and
commercialization of medical products and already have a sales force in place to launch new
products. Consequently, they may be able to develop alternative forms of medical treatment which
could compete with our products and which could be commercialized more rapidly and effectively than
our products.

If we fail to comply with government regulations regarding the import and export of products and
raw materials, we could be subject to fines, sanctions and penalties that could adversely affect
our ability to operate our business.

We import and export products and raw materials from and to several jurisdictions around the
world. This process requires us and our commercial partners to operate in a number of
jurisdictions with different customs and import/export regulations. The regulations of these
countries are subject to change from time to time and we cannot predict the nature, scope or
impact of these changes upon our operations. We and our commercial partners are subject to
periodic reviews and audits by U.S. and foreign authorities responsible for administering these
regulations. To the extent that we or our commercial partners are unable to successfully defend
against an audit or review, we may be required to pay assessments, penalties and increased duties,
which may, individually or in the aggregate, negatively impact our business, operating results and
financial condition.

Risks Related to the Regulatory Review Process

Even after regulatory approval has been obtained regulatory agencies may impose limitations on
the indicated uses for which our products may be marketed, subsequently withdraw approval or take
other actions against us that would be adverse to our business.

Even though we have obtained marketing approval of EGRIFTATM in the United States, the
FDA and regulatory agencies in other countries have the ability to limit the indicated use of a
product. Also, the manufacture, marketing and sale of our products will be subject to ongoing and
extensive governmental regulation in the country in which we intend to market our products. For
example, although we obtained marketing approval of EGRIFTATM for the reduction of
excess abdominal fat in HIV-infected patients with lipodystrophy in the United States, the
marketing of EGRIFTATM will be subject to extensive regulatory requirements
administered by the FDA, such as adverse event reporting and compliance with marketing and
promotional requirements. The FDA has also requested that we comply with certain post-approval
requirements in connection with the approval of EGRIFTATM for the reduction of excess
abdominal fat in HIV-infected patients with lipodystrophy, namely, the development of a single
vial formulation of EGRIFTATM (the development of a new presentation of the same
formulation), a long-term observational

- 28 -

 

safety study using EGRIFTATM; and a Phase 4 clinical trial. Although we have
received marketing approval from the FDA of tesamorelin for the reduction of excess abdominal fat
in HIV-infected patients with lipodystrophy, there can be no guarantee that regulatory agencies in
other countries will approve tesamorelin for this treatment in their respective countries.

Our third party manufacturing facilities for EGRIFTATM will also be subject to
continuous reviews and periodic inspections and approval of manufacturing modifications by
regulatory agencies, including the FDA. The facilities must comply with GMP regulations. The
failure to comply with FDA requirements can result in a series of administrative or judicial
sanctions or other setbacks, including:

	 	•	 	restrictions on the use of the product, manufacturers or manufacturing processes;
	 
	 	•	 	warning letters;
	 
	 	•	 	civil or criminal penalties;
	 
	 	•	 	fines;
	 
	 	•	 	injunctions;
	 
	 	•	 	product seizures or detentions;
	 
	 	•	 	import or export bans or restrictions;
	 
	 	•	 	product recalls and related publicity requirements;
	 
	 	•	 	suspension or withdrawal of regulatory approvals;
	 
	 	•	 	total or partial suspension of production; and
	 
	 	•	 	refusal to approve pending applications for marketing approval of new product candidates or
supplements to approved applications.

Addressing any of the foregoing or any additional requirements of the FDA or other regulatory
authorities may require significant resources and could impair our ability to successfully
commercialize our product candidates.

To date, we do not have the required regulatory approvals to commercialize EGRIFTA
TM
outside of the United States and cannot guarantee that we will obtain such regulatory approvals or
that any of our product candidates will be approved for commercialization in any country, including
the United States.

The commercialization of EGRIFTATM outside of the United States and our future products
first requires the approval of the regulatory agencies in each of the jurisdictions where we intend
to sell such products. In order to obtain the required approvals, we must demonstrate, following
preclinical and clinical studies, the safety, efficacy and quality of a product.

The rules and regulations relating to the approval of a new drug are complex and stringent.
Although we have received marketing approval in the United States from the FDA for
EGRIFTATM, there can be no guarantee that regulatory agencies in other territories will
approve EGRIFTATM in their respective countries.

- 29 -

 

All of our product candidates are subject to preclinical and clinical studies. If the results
of such studies are not positive, we may not be in a position to make any filing to obtain the
regulatory approval for the product candidate or, even where a product candidate has been filed for
approval, we may have to conduct additional clinical trials or testing on such product candidate in
an effort to obtain results that further support the safety and efficacy of such product candidate.
Such studies are often costly and may also delay a filing or, where additional studies or testing
are required after a filing has been made, the approval of a product candidate.

While an application for a new drug is under review by a regulatory agency, it is standard for such
regulatory agency to ask questions regarding the application that was submitted. If these questions
are not answered quickly and in a satisfactory manner, the marketing approval of the product
candidate subject to the review and its commercialization could be delayed or, if the questions are
not answered in a satisfactory manner, denied. If EGRIFTATM is not approved by the
appropriate regulatory agencies for commercialization outside of the United States, our capacity to
generate revenues in the long-term will be impaired and this will have an adverse effect on our
financial condition and our operating results.

Obtaining regulatory approval is subject to the discretion of regulatory agencies in each relevant
jurisdiction. Therefore, even if we obtain regulatory approval from one agency, or succeed in
filing the equivalent of a new drug application, or NDA, in other countries, or have obtained
positive results relating to the safety and efficacy of a product candidate, a regulatory agency
may not accept the filing or the results contained therein as being conclusive evidence of the
safety and efficacy of a product candidate in order to allow us to sell the product candidate in
its country. A regulatory agency may require that additional tests on the safety and efficacy of a
product candidate be conducted prior to granting approval of such product candidate. These
additional tests may delay the approval of such product candidate, can have a material adverse
effect on our financial condition and results of operations based on the type of additional tests
to be conducted and may not necessarily lead to the approval of the product candidate.

We have only obtained FDA approval for EGRIFTA
TM and we must complete several
preclinical studies and clinical trials for our other product candidates which may not yield
positive results and, consequently, could prevent us from obtaining regulatory approval.

If any of our preclinical studies or clinical trials fail to show positive efficacy data or result
in adverse patient reactions, we may be required to perform additional preclinical studies or
clinical trials, to extend the term of our studies and trials, to increase the number of patients
enrolled in a given trial or to undertake ancillary testing. Any of these events could cause an
increase in the cost of product development, delay filing of an application for marketing approval
or result in the termination of a study or trial and, accordingly, could cause us to cease the
development of a product candidate. In addition, the future growth of our business could be
negatively impacted since there can be no guarantee that we will be able to develop new compounds,
license or purchase compounds or product candidates that will result in marketed products.

Recently enacted and future legislation may increase the difficulty and cost for us to obtain
marketing approval of and commercialize our product candidates and affect the prices we may obtain.

In the United States and some foreign jurisdictions, there have been a number of legislative and
regulatory changes and proposed changes regarding the healthcare system that could prevent or delay
marketing approval for our product candidates, restrict or regulate post-approval

- 30 -

 

activities and affect our ability to profitably sell EGRIFTATM or any of our other
product candidates for which we intend to seek marketing approval.

Legislative and regulatory proposals have been made to expand post-approval requirements and
restrict sales and promotional activities for pharmaceutical products. We are not sure whether
additional legislative changes will be enacted, or whether the FDA regulations, guidance or
interpretations will be changed, or what the impact of such changes on the marketing approvals of
our product candidates, if any, may be. In addition, increased scrutiny by the U.S. Congress of the
FDA’s approval process may significantly delay or prevent marketing approval, as well as subject us
to more stringent product labeling and post-marketing testing and other requirements.

In the United States, the Medicare Modernization Act, or MMA, changed the way Medicare covers and
pays for pharmaceutical products. The legislation expanded Medicare coverage for drug purchases by
the elderly and introduced a new reimbursement methodology based on average sales prices for drugs.
In addition, this legislation authorized Medicare Part D prescription drug plans to use formularies
where they can limit the number of drugs that will be covered in any therapeutic class. As a result
of this legislation and the expansion of federal coverage of drug products, we expect that there
will be additional pressure to contain and reduce costs. These cost reduction initiatives and other
provisions of this legislation could decrease the coverage and sales price that we receive for
EGRIFTATM or any other approved products and could seriously harm our business. While
the MMA applies only to drug benefits for Medicare beneficiaries, private payors often follow
Medicare coverage policy and payment limitations in setting their own reimbursement rates, and any
reduction in reimbursement that results from the MMA may result in a similar reduction in payments
from private payors.

More recently, in March 2010, U.S. President Obama signed into law the Health Care Reform Law, a
sweeping law intended to broaden access to health insurance, reduce or constrain the growth of
healthcare spending, enhance remedies against fraud and abuse, add new transparency requirements
for healthcare and health insurance industries, impose new taxes and fees on the health industry
and impose additional health policy reforms. Effective October 1, 2010, the Health Care Reform Law
revised the definition of “average manufacturer price” for reporting purposes, which could increase
the amount of Medicaid drug rebates to states. Further, beginning in 2011, the new law imposes a
significant annual fee on companies that manufacture or import branded prescription drug products.
We will not know the full effects of the Health Care Reform Law until applicable U.S. federal and
state agencies issue regulations or guidance under the new law. Although it is too early to
determine the effect of the Health Care Reform Law, the new law appears likely to continue to apply
the pressure on pharmaceutical pricing. Pressure on pharmaceutical pricing may adversely affect the
amount of our royalties in the United States.

Risks Related to Our Intellectual Property

Our failure to protect our intellectual property may have a material adverse effect on our
ability to develop and commercialize our products.

We will be able to protect our intellectual property rights from unauthorized use by third parties
only to the extent that our intellectual property rights are covered and protected by valid and
enforceable patents or are effectively maintained as trade secrets. We try to protect our
intellectual property position by, among other things, filing patent applications related to our

- 31 -

 

proprietary technologies, inventions and improvements that are important to the development of
our business.

Because the patent position of pharmaceutical companies involves complex legal and factual
questions, the issuance, scope, validity, and enforceability of patents cannot be predicted with
certainty. Patents, if issued, may be challenged, invalidated or circumvented. If our patents are
invalidated or found to be unenforceable, we would lose the ability to exclude others from making,
using or selling the inventions claimed. Moreover, an issued patent does not guarantee us the right
to use the patented technology or commercialize a product using that technology. Third parties may
have blocking patents that could be used to prevent us from developing our product candidates,
selling our products or commercializing our patented technology. Thus, patents that we own may not
allow us to exploit the rights conferred by our intellectual property protection.

Our pending patent applications may not be issued or granted as patents. Even if issued, they may
not be issued with claims of sufficient breadth to protect our product candidates and technologies
or may not provide us with a competitive advantage against competitors with similar products or
technologies. Furthermore, others may independently develop products or technologies similar to
those that we have developed or may reverse engineer or discover our trade secrets through proper
means. In addition, the laws of many countries do not protect intellectual property rights to the
same extent as the laws of Canada, the United States and the European Patent Convention, and those
countries may also lack adequate rules and procedures for defending intellectual property rights
effectively.

Although we have received patents from the United States Patent and Trademark Office, or USPTO, for
the treatment of HIV-related lipodystrophy with tesamorelin, there can be no guarantee that, in the
other countries where we filed patent applications for the treatment of HIV-related lipodystrophy,
we will receive a patent or obtain granted claims of similar breadth to those granted by the USPTO.

We also rely on trade secrets, know-how and technology, which are not protected by patents, to
maintain our competitive position. We try to protect this information by entering into
confidentiality agreements with parties who have access to such confidential information, such as
our current and prospective suppliers, distributors, manufacturers, commercial partners, employees
and consultants. Any of these parties may breach the agreements and disclose confidential
information to our competitors. It is possible that a competitor will make use of such information,
and that our competitive position could be disadvantaged.

Enforcing a claim that a third party infringes on, has illegally obtained or is using an
intellectual property right, including a trade secret or know-how, is expensive and time-consuming
and the outcome is unpredictable. In addition, enforcing such a claim could divert management’s
attention from our business. If any intellectual property right were to be infringed, disclosed to
or independently developed by a competitor, our competitive position could be harmed. Any adverse
outcome of such litigation or settlement of such a dispute could subject us to significant
liabilities, could put one or more of our patents at risk of being invalidated or interpreted
narrowly, could put one or more of our patents at risk of not issuing, or could facilitate the
entry of generic products. Any such litigation
could also divert our research, technical and management personnel from their normal
responsibilities.

Our ability to defend ourselves against infringement by third parties of our intellectual property
in the United States with respect to tesamorelin for the treatment of HIV-related lipodystrophy

- 32 -

 

depends, in part, on our commercial partner’s decision to bring an action against such third
party. Under the terms and conditions of our collaboration and licensing agreement with EMD Serono,
EMD Serono has the first right to bring an action against a third party for infringing our patent
rights with respect to tesamorelin for the treatment of HIV-related lipodystrophy. Any delay in
pursuing such action or in advising us that it does not intend to pursue the matter could decrease
sales, if any, of tesamorelin for the treatment of HIV-related lipodystrophy and adversely affect
our revenues.

Furthermore, because of the substantial amount of discovery required in connection with
intellectual property litigation, there is a risk that some of our confidential information could
be compromised by disclosure during this type of litigation. For example, confidential information
may be disclosed, inadvertently or as ordered by the court, in the form of documents or testimony
in connection with discovery requests, depositions or trial testimony. This disclosure would
provide our competitors with access to our proprietary information and may harm our competitive
position.

Our commercial success depends, in part, on our ability not to infringe on third party patents and
other intellectual property rights.

Our capacity to commercialize our product candidates, and more particularly tesamorelin, will
depend, in part, upon our ability to avoid infringing third party patents and other third party
intellectual property rights. The biopharmaceutical and pharmaceutical industries have produced a
multitude of patents and it is not always easy for participants, including us, to determine which
patents cover various types of products, processes of manufacture or methods of use. The scope and
breadth of patents is subject to interpretation by the courts and such interpretation may vary
depending on the jurisdiction where the claim is filed and the court where such claim is litigated.
The fact that we own patents for tesamorelin and for the treatment of HIV-related lipodystrophy
does not guarantee that we are not infringing one or more third-party patents and there can be no
guarantee that we will not infringe or violate third-party patents and other third-party
intellectual property rights in the United States or other jurisdictions.

Patent analysis for non-infringement is based in part on a review of publicly available databases.
Although we review from time to time certain databases to conduct patent searches, we do not have
access to all databases. It is also possible that we will not have reviewed some of the information
contained in the databases or we found it to be irrelevant at the time we conducted the searches.
In addition, because patents take years to issue, there may be currently pending applications that
have not yet been published or that we are unaware of, which may issue later as patents. As a
result, there can be no guarantee that we will not violate third-party patents.

Because of the difficulty in analyzing and interpreting patents, there can be no guarantee that a
third party will not assert that we infringe such third-party’s patents or any of its other
intellectual property rights. Under such circumstances, there is no guarantee that we would not
become involved in litigation. Litigation with any third party, even if the allegations are without
merit, is expensive, time-consuming and would divert management’s attention from the daily
execution of our business plan. Litigation implies that a portion of our financial assets would be
used to sustain the costs of litigation instead of being allocated to further the development of
our business.

If we are involved in patent infringement litigation, we would need to prevail in demonstrating
that our products do not infringe the asserted patent claims of the relevant patent, that the
patent claims are invalid or that the patent is unenforceable. If we are found to infringe a
third-party

- 33 -

 

patent or other intellectual property right, we could be required to enter into royalty or
licensing agreements on terms and conditions that may not be favourable to us, and/or pay damages,
including up to treble damages in the United Sates (for example, if found liable of wilful
infringement) and/or cease the development and commercialization of our product candidates. Even if
we were able to obtain a license, the rights may be nonexclusive, which could result in our
competitors gaining access to the same intellectual property and to compete with us.

We have not been served with any notice alleging that we infringe a third-party patent, but there
may be issued patents that we are unaware of that our products may infringe, or patents that we
believe we do not infringe but ultimately could be found to infringe. We are aware of third-party
patents for the reduction of accumulation of fat tissue in HIV patients and, if a patent
infringement suit was brought against us, we believe that we should not be found to infringe any
valid claims of these patents. If we were to challenge the validity of a competitor’s issued United
States patent in a United States court, we would need to overcome a statutory presumption of
validity that attaches to every United States patent. This means that, in order to prevail, we
would have to present clear and convincing evidence as to the invalidity of the patent’s claims. We
cannot guarantee that a court would find in our favour on questions of infringement and validity.
Any finding that we infringe or violate a third-party patent or other intellectual property right
could materially adversely affect our business, financial condition and operating results.

Other Risks Related to Our Business

We have a history of net losses and we may never achieve high profitability.

We have been reporting losses since our inception (except for the financial years ended November
30, 2010, 2001 and 2000) and, as at November 30, 2010, we had an accumulated deficit of
$235,116,000. We do not expect to generate significant recurrent revenues sufficient to cover our
overall activities in the immediate future. As a result of the foregoing, we will need to generate
significant revenues to achieve profitability.

Our profitability will depend on, among other things, our commercial partners’ ability and
willingness to successfully commercialize EGRIFTATM and to obtain regulatory approval
for the use of tesamorelin in the reduction of excess abdominal fat in HIV-infected patients with
lipodystrophy in Europe, Latin America, Africa and the Middle East. However, there is no guarantee
that our commercial partners will succeed in commercializing EGRIFTATM or that our
product candidates will ever receive approval for commercialization in any jurisdiction and,
accordingly, we may never sustain profitability.

We rely on third-party service providers to conduct our preclinical studies and clinical trials and
the failure by any of these third parties to comply with their obligations may delay the studies
which could have an adverse effect on our development programs.

We have limited human resources to conduct preclinical studies and clinical trials and must rely on
third-party service providers to conduct our studies and trials and carry out certain data
gathering and analyses. If our third-party service providers become unavailable for any reason,
including as a result of the failure to comply with the rules and regulations governing the conduct
of preclinical studies and clinical trials,
operational failures such as equipment failures or unplanned facility shutdowns, or damage from any
event such as fire, flood, earthquake, business restructuring or insolvency or, if they fail to
perform their contractual obligations pursuant to the terms of our agreements with them, such as
failing to perform the testing,

- 34 -

 

compute the data or complete the reports further to the testing, we may incur delays which may
be significant in connection with the planned timing of our trials and studies which could
adversely affect the timing of the development program of a product candidate or the filing of an
application for marketing approval in a jurisdiction where we rely on third-party service providers
to make such filing. In addition, where we rely on such third-party service provider to help in
answering any question raised by a regulatory agency during its review of one of our files, the
unavailability of such third-party service provider may adversely affect the timing of the review
of an application and, could ultimately delay the approval. If the damages to any of our
third-party service providers are material, or, for any reason, such providers do not operate in
compliance with Good Laboratory Practices, or GLP, or are unable or refuse to perform their
contractual obligations, we would need to find alternative third-party service providers.

If we needed to change or select new third-party service providers, the planned working schedule
related to preclinical studies and/or clinical trials could be delayed since the number of
competent and reliable third-party service providers of preclinical and clinical work in compliance
with GLP is limited. In addition, if we needed to change or select new third-party service
providers to carry out work in response to a regulatory agency review of one of our applications,
there may be delays in responding to such regulatory agency which, in turn, may lead to delays in
commercializing a product candidate.

Any selection of new third-party service providers to carry out work related to preclinical studies
and clinical trials would be time-consuming and would result in additional delays in receiving
data, analysis and reports from such third-party service providers which, in turn, would delay the
filing of any new drug application with regulatory agencies for the purposes of obtaining
regulatory approval to commercialize our product candidates. Furthermore, such delays could
increase our expenditures to develop a product candidate and materially adversely affect our
financial condition and operating results.

The conduct of clinical trials requires the enrolment of patients and difficulties in enrolling
patients could delay the conduct of our clinical trials or result in their non-completion.

The conduct of clinical trials requires the enrolment of patients. We may have difficulties
enrolling patients for the conduct of our future clinical trials as a result of design protocol,
the size of the patient population, the eligibility criteria to participate in the clinical trials,
the availability of competing therapies, the patient referral practices of physicians and the
availability of clinical trial sites. Difficulty in enrolling patients for our clinical trials
could result in the cancellation of clinical trials or delays in completing them. Once patients are
enrolled in a clinical trial, the occurrence of any adverse drug effects or side effects observed
during the trial could result in the clinical trial being cancelled. Any of these events would have
material adverse consequences on the timely development of our product candidates, the filing of an
NDA, or its equivalent, with regulatory agencies and the commercialization of such product
candidates.

We may require additional funding and may not be able to raise the capital necessary to fund all or
part of our capital requirements, including to continue and complete the research and development
of our product candidates and their commercialization.

We do not generate significant recurrent revenues and may need financing in order to fund all or
part of our capital requirements to sustain our growth, to continue research and development of new
product candidates, to conduct clinical programs, to develop our marketing and commercial
capabilities and to meet our compliance obligations with various rules and regulations to which

- 35 -

 

we are subject. In the past, we have been financed through public equity offerings in Canada
and private placements of our equity securities and we may need to seek additional equity offerings
to raise capital, the size of which cannot be predicted. However, the market conditions or our
business performance may prevent us from having access to the public market in the future at the
times or in the amounts necessary. Therefore, there can be no guarantee that we will be able to
continue to raise additional equity capital by way of public or private equity offerings in the
future. In such a case, we would have to use other means of financing, such as issuing debt
instruments or entering into private financing or credit agreements, the terms and conditions of
which may not be favorable to us. If adequate funding is not available to us, we may be required to
delay, reduce, or eliminate our research and development of new product candidates, our clinical
trials or our marketing and commercialization efforts to launch and distribute new products,
curtail significant portions of our product development programs that are designed to identify new
product candidates and sell or assign rights to our technologies, products or product candidates.
In addition, the issuance and sale of substantial amounts of equity, or other securities, or the
perception that such issuances and sales may occur could adversely affect the market price of our
common shares.

If product liability lawsuits are brought against us, they could result in costly and
time-consuming litigation and significant liabilities.

Despite all reasonable efforts to ensure the safety of EGRIFTATM and our other product
candidates, it is possible that we or our commercial partners will sell products which are
defective, to which patients react in an unexpected manner, or which are alleged to have side
effects. The manufacture and sale of such products may expose us to potential liability, and the
industries in which our products are likely to be sold have been subject to significant product
liability litigation. Any claims, with or without merit, could result in costly litigation, reduced
sales, significant liabilities and diversion of our management’s time and attention and could have
a material adverse effect on our financial condition, business and results of operations.

If a product liability claim is brought against us, we may be required to pay legal and other
expenses to defend the claim and, if the claim is successful, damage awards may be substantial
and/or may not be covered, in whole or in part, by our insurance. We may not have sufficient
capital resources to pay a judgment, in which case our creditors could levy against our assets. We
may also be obligated to indemnify our commercial partners and make payments to other parties with
respect to product liability damages and claims. Defending any product liability claims, or
indemnifying others against those claims, could require us to expend significant financial and
managerial resources.

The development and commercialization of our drugs could expose us to liability claims which could
exceed our insurance coverage.

A risk of product liability claims is inherent in the development and commercialization of human
therapeutic products. Product liability insurance is very expensive and offers limited protection.
A product liability claim against us could potentially be greater than the available coverage and,
therefore, have a material adverse effect upon us and our financial condition. Furthermore, a
product liability claim could tarnish our reputation, whether or not such claims are covered by
insurance or are with or without merit.

We depend on our key personnel to research, develop and bring new products to the market and the
loss of key personnel or the inability to attract highly qualified individuals could have a
material adverse effect on our business and growth potential.

- 36 -

 

The operation of our business requires qualified scientific and management personnel. The loss of
scientific personnel or members of management could have a material adverse effect on our business.
In addition, our growth is and will continue to be dependent, in part, on our ability to hire and
retain the employment of qualified personnel. There can be no guarantee that we will be able to
continue to retain our current employees or will be able to attract qualified personnel to achieve
our business plan.

We may be unable to identify and complete in-licensing or acquisitions. In-licensing or
acquisitions could divert management’s attention and financial resources, may negatively affect our
operating results and could cause significant dilution to our shareholders.

In the future, we may engage in selective in-licensing or acquisitions of products or businesses
that we believe are complementary to our products or business. There is a risk that we will not be
able to identify suitable in-licensing or acquisition candidates available for sale at reasonable
prices, complete any in-licensing or acquisition, or successfully integrate any in-licensed or
acquired product or business into our operations. We are likely to face competition for
in-licensing or acquisition candidates from other parties including those that have substantially
greater available resources. In-licensing or acquisitions may involve a number of other risks,
including:

	 	•	 	diversion of management’s attention;
	 
	 	•	 	disruption to our ongoing business;
	 
	 	•	 	
failure to retain key acquired personnel; 
	 
	 	•	 	difficulties in integrating acquired
operations, technologies, products or personnel; 
	 
	 	•	 	 unanticipated expenses, events or
circumstances; 
	 
	 	•	 	 assumption of disclosed and undisclosed liabilities;
	 
	 	•	 	inappropriate valuation of the acquired in-process research and development, or the
entire acquired business; and
	 
	 	•	 	difficulties in maintaining customer relations.

If we do not successfully address these risks or any other problems encountered in connection with
an acquisition, the acquisition could have a material adverse effect on our business, results of
operations and financial condition. Inherited liabilities of or other issues with an acquired
business could have a material adverse effect on our performance or our business as a whole. In
addition, if we proceed with an acquisition, our available cash may be used to complete the
transaction, diminishing our liquidity and capital resources, or shares may be issued which could
cause significant dilution to our existing shareholders.

We may not achieve our publicly announced milestones on time.

From time to time, we publicly announce the timing of certain events to occur. These statements are
forward-looking and are based on the best estimate of management at the time relating to

- 37 -

 

the occurrence of such events. However, the actual timing of such events may differ from what has
been publicly disclosed. Events such as completion of a clinical program, discovery of a new
product candidate, filing of an application to obtain regulatory approval, beginning of
commercialization of our products or announcement of additional clinical programs for a product
candidate may vary from what is publicly disclosed. These variations may occur as a result of a
series of events, including the nature of the results obtained during a clinical trial or during a
research phase, problems with a supplier or a commercial partner or any other event having the
effect of delaying the publicly announced timeline. Our policy on disclosure of forward-looking
information consists of not updating it if the publicly disclosed timeline varies, except as may be
required by law. Any variation in the timing of certain events having the effect of postponing such
events could have an adverse material effect on our business plan, financial condition or operating
results.

The outcome of scientific research is uncertain and our failure to discover new compounds could
slow down the growth of our portfolio of products.

We conduct research activities in order to increase our portfolio of product candidates. The
outcome of scientific research is uncertain and may prove unsuccessful and, therefore, may not lead
to the discovery of new molecules and progression of existing compounds to an advanced development
stage. Our inability to develop new compounds or to further develop the existing ones could slow
down the growth of our portfolio of products.

Risks Related to our Common Shares

Our share price has been volatile, and an investment in our common shares could suffer a
decline in value.

Since our initial public offering in Canada, our valuation and share price have had no meaningful
relationship to current or historical financial results, asset values, book value or many other
criteria based on conventional measures of the value of common shares. The market price of our
common shares will fluctuate due to various factors including the risk factors described herein and
other facts beyond our control.

In the past, when the market price of a stock has been volatile, shareholders have often instituted
securities class action litigation against that company. If any of our shareholders brought a
lawsuit against us, we could incur substantial costs defending the lawsuit. The lawsuit could also
divert the time and attention of our management.

Our quarterly operating results may fluctuate significantly.

We expect our operating results to be subject to quarterly fluctuations. Our net loss and other
operating results will be affected by numerous factors, including:

	 	•	 	variations in the level of revenues and royalties received related to our
development programs;
	 
	 	•	 	variations in the level of expenses related to our development programs;
	 
	 	•	 	addition or termination of clinical trials;

- 38 -

 

	 	•	 	any intellectual property infringement lawsuit in which we may become involved;
	 
	 	•	 	regulatory developments affecting our product candidates;
	 
	 	•	 	our execution of any collaborative, licensing or similar arrangements, and the
timing of payments we may make or receive under these arrangements; and
	 
	 	•	 	the achievement and timing of milestone payments under our existing strategic
partnership agreements.

If our quarterly operating results fall below the expectations of investors or securities analysts,
the price of our common shares could decline substantially. Furthermore, any quarterly fluctuations
in our operating results may, in turn, cause the price of our stock to fluctuate substantially.

We do not intend to pay dividends on our common shares and, consequently, your ability to achieve a
return on your investment will depend on appreciation in the price of our common shares.

We have never declared or paid any cash dividend on our common shares and do not currently intend
to do so for the foreseeable future. We currently anticipate that we will retain future earnings
for the development, operation and expansion of our business and do not anticipate declaring or
paying any cash dividends for the foreseeable future. Therefore, the success of an investment in
our common shares will depend upon any future appreciation in their value. There is no guarantee
that our common shares will appreciate in value or even maintain the price at which our
shareholders have purchased their shares.

Our revenues and expenses may fluctuate significantly and any failure to meet financial
expectations may disappoint securities analysts or investors and result in a decline in the price
of our common shares.

Our revenues and expenses have fluctuated in the past and are likely to do so in the future. These
fluctuations could cause our share price to decline. Some of the factors that could cause revenues
and expenses to fluctuate include the following:

	 	•	 	the inability to complete product development in a timely manner that results in a
failure or delay in receiving the required regulatory approvals or allowances to
commercialize product candidates;
	 
	 	•	 	the timing of regulatory submissions and approvals;
	 
	 	•	 	the timing and willingness of any current or future collaborators to invest the
resources necessary to commercialize the product candidates;
	 
	 	•	 	the outcome of any litigation;
	 
	 	•	 	changes in foreign currency fluctuations;
	 
	 	•	 	the timing of achievement and the receipt of milestone payments from current or
future third parties;

- 39 -

 

	 	•	 	failure to enter into new or the expiration or termination of current agreements
with third parties; and
	 
	 	•	 	failure to introduce the product candidates to the market in a manner that generates
anticipated revenues.

We may be adversely affected by currency fluctuations.

A substantial portion of our revenue is earned in U.S. dollars, but a substantial portion of our
operating expenses are incurred in Canadian dollars. Fluctuations in the exchange rate between the
U.S. dollar and other currencies, such as the Canadian dollar, may have a material adverse effect
on our business, financial condition and operating results. We do not currently engage in
transactional hedging schemes but we do attempt to hedge or mitigate the risk of currency
fluctuations by actively monitoring and managing our foreign currency holdings relative to our
foreign currency expenses.

Our articles and certain Canadian laws could delay or deter a change of control.

On February 10, 2010, we entered into a shareholder rights plan agreement. In the event of certain
change of control transactions, the plan entitles a rights holder, other than the person or group
acquiring control, to subscribe to our common shares at a discount of 50 percent to the market
price at that time, subject to certain exceptions.

The Investment Canada Act (Canada) subjects an acquisition of control of a company by a
non-Canadian to government review if the value of the assets as calculated pursuant to the
legislation exceeds a threshold amount. A reviewable acquisition may not proceed unless the
relevant minister is satisfied that the investment is likely to be a net benefit to Canada.

Any of the foregoing could prevent or delay a change of control and may deprive or limit strategic
opportunities for our shareholders to sell their shares.

Further information on Theratechnologies

Further information on Theratechnologies, including the Company’s Annual Information Form, is
available on the SEDAR site at www.sedar.com.

- 40 -

Source: [{"source": "alea-institute/alea-institute/kl3m-data-edgar-agreements/train-00184-of-00352.parquet"}, [{"source": "alea-institute/alea-institute/kl3m-data-edgar-agreements/train-00184-of-00352.parquet"}]]