Source: EURLEX
Language: en
Format: md

OPINION OF ADVOCATE GENERAL

MENGOZZI

delivered on 31 March 2011 ([1](#Footnote1))

**Case C‑195/09**

**Synthon BV**

**v**

**Merz Pharma GmbH & Co. KGaA**

(Reference for a preliminary ruling from the High Court of Justice (Chancery Division) (United Kingdom))

(Regulation No 1768/92 – Supplementary protection certificate – Conditions for its grant – Concept of first marketing authorisation)

  
  
  
  

1.        Under the Community harmonising legislation concerning medicinal products, such products may be placed on the market only
on completion of a lengthy authorisation procedure, introduced in order to prot ect public health. As a result, there are
cases in which it may not be possible to begin exploiting patents for medicinal products until several years after they have
been conferred. Introduced by Regulation 1768/92, ([2](#Footnote2)) the supplementary protection certificate (SPC) is designed specifically to limit the extent to which the period of exclusive
use of such patents may be eroded. ([3](#Footnote3))

2.        In this case, four questions for a preliminary ruling have been raised concerning the interpretation of Articles 13 and 19
of the regulation. Those questions arose in the context of a dispute between Synthon BV (‘Synthon’) and Merz Pharma GmbH &
Co KGaA (‘Merz’) concerning the validity and term of an SPC granted to Merz by the United Kingdom Trade Mark Office for an
active ingredient which had already been present on the market for several years, although as an ingredient in a medicinal
product used for different therapeutic purposes from those described in the basic patent. In essence, the national court asks
the Court of Justice to clarify whether the authorisations to place that medicinal product on the market, which were accorded
to Merz in two Member States without the product’s being subjected to the tests of efficacy and safety required under Community
harmonising legislation, must, in any event, be taken into account in determining the validity and term of the SPC granted
to Merz.

I –  **Legislative background**

A –    *European Union law*

1.      Directives 65/65/EEC and 75/319/EEC

3.        According to Article 3 of Council Directive 65/65/EEC of 26 January 1965 ([4](#Footnote4)) on the approximation of provisions laid down by law, regulation or administrative action relating to proprietary medicinal
products, in the version applicable to the facts of the main proceedings, ([5](#Footnote5)) no proprietary medicinal product ([6](#Footnote6)) may be placed on the market in a Member State unless an authorisation has been issued by the competent authority of that
Member State.

4.        In order to obtain that authorisation, the person responsible for placing the product on the market had to submit to the competent
authority of the Member State concerned an application supported by the particulars and documents specified in Article 4(2)
of the directive. As well as information such as the qualitative and quantitative particulars of all the constituents of the
proprietary product, a brief description of the method of preparation, the therapeutic indications, contra-indications and
side-effects, posology and a description of the control methods employed by the manufacturer, Article 4(8) of the directive
listed, among the particulars and documents that were to accompany the application, the results of physico-chemical, biological
or microbiological tests, pharmacological and toxicological tests and clinical trials.

5.        Directive 75/319 ([7](#Footnote7)) laid down the procedures to be used by the Member States when examining SPC applications. These included, in particular,
the possibility of submitting the proprietary medicinal product for testing by a State laboratory and of requesting additional
documentation.

6.        According to Article 5 of Directive 65/65:

‘The authorisation provided for in Article 3 shall be refused if, after verification of the particulars and documents listed
in Article 4, it proves that the medicinal product is harmful in the normal conditions of use, or that its therapeutic efficacy
is lacking or is insufficiently substantiated by the applicant, or that its qualitative and quantitative composition is not
as declared’.

7.        According to Article 24 of Directive 65/65, as replaced by Article 37 of Directive 75/319:

‘Within the time limits and under the conditions laid down in Article 39(2) and (3) of second Directive 75/319/EEC, the rules
laid down in this directive shall be applied progressively to proprietary medicinal products covered by an authorisation to
place on the market by virtue of previous provisions’.

8.        According to Article 39(2) and (3) of Directive 75/319:

‘2. Within 15 years of the notification referred to in Article 38, the other provisions of this directive shall be applied
progressively to proprietary medicinal products placed on the market by virtue of previous provisions.

 3. Member States shall notify the Commission, within three years following the notification of this Directive, of the number
of proprietary medicinal products covered by paragraph 2, and, each subsequent year, of the number of these products for which
a marketing authorisation referred to in Article 3 of Directive 65/65/EEC, has not yet been issued’.

9.        According to Article 22 of Directive 65/65, ‘Member States shall put into force the measures needed in order to comply with
this directive within 18 months of its notification ([8](#Footnote8)) and shall inform the Commission forthwith’.

2.      Regulation No 1768/92

10.      The reason for extending the duration of the protection conferred by the patent in the case of medicinal products is set out
in the preamble to Regulation No 1768/92 ([9](#Footnote9)) (‘the regulation’). According to recitals 3, 4, 6 and 7 in particular:

‘[w]hereas at the moment the period that elapses between the filing of an application for a patent for a new medicinal product
and authorisation to place the medicinal product on the market makes the period of effective protection under the patent insufficient
to cover the investment put into the research;

[w]hereas this situation leads to a lack of protection which penalises pharmaceutical research;

...

[w]hereas a uniform solution at Community level should be provided for, thereby preventing the heterogeneous development of
national laws leading to further disparities which would be likely to create obstacles to the free movement of medicinal products
within the Community and thus directly affect the establishment and functioning of the internal market;

[w]hereas, therefore, the creation of a supplementary protection certificate granted, under the same conditions, by each of
the Member States at the request of the holder of a national or European patent relating to a medicinal product for which
marketing authorisation has been granted is necessary; whereas a regulation is therefore the most appropriate legal instrument;

11.      Under Article 1 of the regulation:

‘[f]or the purposes of this regulation:

(a) “medicinal product” means any substance or combination of substances presented for treating or preventing disease in human
beings or animals and any substance or combination of substances which may be administered to human beings or animals with
a view to making a medical diagnosis or to restoring, correcting or modifying physiological functions in humans or in animals;

(b) “product” means the active ingredient or combination of active ingredients of a medicinal product;

(c) “basic patent” means a patent which protects as defined in (b) as such, a process to obtain a product or an application
of a product, and which is designated by its holder for the purpose of the procedure for grant of a certificate’.

12.      Article 2 of the regulation, entitled ‘Scope’ provides:

‘Any product protected by a patent in the territory of a Member State and subject, prior to being placed on the market as
a medicinal product, to an administrative authorization procedure as laid down in ... Directive 65/65 ... may, under the terms
and conditions provided for in this regulation, be the subject of a certificate’.

13.      Under Article 3 of the regulation, entitled ‘Conditions for obtaining a certificate’:

‘A certificate shall be granted if, in the Member State in which the application referred to in Article 7 is submitted and
at the date of that application:

(a) the product is protected by a basic patent in force;

(b) a valid authorisation to place the product on the market as a medicinal product has been granted in accordance with Directive
65/65/EEC ... . For the purpose of Article 19 (1), an authorisation to place the product on the market granted in accordance
with the national legislation of Austria, Finland, or Sweden is treated as an authorisation granted in accordance with Directive
65/65/EEC;

(c) the product has not already been the subject of a certificate;

(d) the authorisation referred to in (b) is the first authorisation to place the product on the market as a medicinal product’.

14.      Pursuant to Article 4 of the regulation, the protection conferred by a certificate is to extend only to the product covered
by the marketing authorisation for the corresponding medicinal product and for any use of the product as a medicinal product
that has been authorised before the expiry of the certificate.

15.      Under Article 7(1) and (2) of the regulation, the application for a certificate is to be lodged within six months of the date
on which the authorisation to place the product on the market was granted or within six months of the date on which the basic
patent was granted, if later.

16.      Under Article 8(1)(a), (b) and (c) of the regulation:

‘The application for a certificate shall contain:

(a) a request for the grant of a certificate, stating in particular:

...

(iii) the number of the basic patent and the title of the invention;

(iv) the number and date of the first authorisation to place the product on the market, as referred to in Article 3 (b) and,
if this authorisation is not the first authorisation for placing the product on the market in the Community, the number and
date of that authorisation;

(b) a copy of the authorisation to place the product on the market, as referred to in Article 3(b), in which the product is
identified, containing in particular the number and date of the authorisation and the summary of the product characteristics
listed in Article 4a of Directive 65/65/EEC ...;

(c) if the authorisation referred to in (b) is not the first authorisation for placing the product on the market as a medicinal
product in the Community, information regarding the identity of the product thus authorised and the legal provision under
which the authorisation procedure took place, together with a copy of the notice publishing the authorisation in the appropriate
official publication’.

17.      Under Article 9(1) of the regulation, the application for a certificate must be lodged with the competent industrial property
office of the Member State which granted the basic patent or on whose behalf it was granted and in which the authorisation
referred to in Article 3(b) to place the product on the market was obtained. Under Article 9(2), notification of the application
for a certificate is be published by the authority referred to in paragraph 1, and must state, inter alia, the number and
date of the authorisation to place the product on the market, referred to in Article 3(b), as well as the product identified
in that authorisation (Article 9(1)(d)) and, where relevant, the number and date of the first authorisation to place the product
on the market in the Community (Article 9(1)(e)). Under Article 11, the same information must appear in the publication containing
the notification of the fact that a certificate has been granted.

18.      Article 13(1) and (2) of the regulation, entitled ‘Duration of the certificate’:

‘1. The certificate shall take effect at the end of the lawful term of the basic patent for a period equal to the period which
elapsed between the date on which the application for a basic patent was lodged and the date of the first authorisation to
place the product on the market in the Community reduced by a period of five years.

2. Notwithstanding paragraph 1, the duration of the certificate may not exceed five years from the date on which it takes
effect’.

19.      Article 15 of the regulation sets out the reasons for which a certificate is invalid. According to Article 15(1):

‘1. The certificate shall be invalid if:

(a) it was granted contrary to the provisions of Article 3;

(b) the basic patent has lapsed before its lawful term expires;

(c) the basic patent is revoked or limited to the extent that the product for which the certificate was granted would no longer
be protected by the claims of the basic patent or, after the basic patent has expired, grounds for revocation exist which
would have justified such revocation or limitation’.

20.      Finally, in its original version, ([10](#Footnote10)) Article 19(1) laid down the following transitional provision:

‘Any product which, on the date on which this regulation enters into force, is protected by a valid basic patent and for which
the first authorisation to place it on the market as a medicinal product in the Community was obtained after 1 January 1985
may be granted a certificate’.

B –    *National legislation*

21.      In Germany, Directive 65/65 was transposed by the Gesetz zur Neuordnung des Arzneimittelrechts of 24 August 1976 (Law restructuring
the legislation on medicinal products: the ‘AMG 1976’). Under Article 3(7) of the AMG 1976, medicinal products which were
present on the market on 1 September 1976, the date of its publication, and were still on the market on 1 January 1978, the
date of its entry into force, automatically continued to be authorised for a period of 12 years, subject to notification.
Under the system previously in force, the placing of medicinal products on the market was not subject to any test of efficacy
and/or safety.

22.      In Luxembourg, the directive was transposed by the grand-ducal regulation of 29 April 1983 implementing the Law of 11 April
1983 regulating the placing on the market and advertising of proprietary medicinal products and ready-made medicinal products
(Loi portant réglementation de la mise sur le marché et de la publicité des spécialités pharmaceutiques et des médicaments
préfabriqués). Article 3 of the law makes the placing on the market of a proprietary medicinal product or ready-made medicinal
product subject to the grant of prior authorisation by the Ministry of Health.

II –  **The dispute in the main proceedings and the questions referred**

23.      Before 1 September 1976, Memantine was marketed in Germany, under the trade mark Akatinol, ([11](#Footnote11)) in accordance with the system in force at that time. On application from Merz, the trade mark holder and defendant in the
main proceedings, the placing on the market of Akatinol was authorised on the basis of Article 3(7) of the AMG 1976. Granted
as of 26 June 1976, that authorisation to place Akatinol on the market (‘the German marketing authorisation’) expired on 1
January 1990. ([12](#Footnote12)) Akatinol appears, however, to have remained on the market in Germany until 9 July 2002.

24.      On 30 June 1983, Merz applied for authorisation to place memantine on the market in Luxembourg. That authorisation was obtained
from the Luxembourg Ministry of Health on 19 September 1983. Despite the fact that the grand-ducal regulation, cited at point
22 above, had already entered into force, the authorisation (‘the Luxembourg marketing authorisation’) was granted without
carrying out the product efficacy and safety tests required under Directive 65/65, and was based solely on the earlier German
authorisation.

25.      On 14 April 1989, Merz applied for a European patent for the product memantine hydrochloride. According to Merz, in its written
observations, its patent application comprised two separate claims for uses of adamantine derivatives (for the preparation
of drugs to treat brain cell lesions caused by cerebral ischemia and for the preparation of a drug to treat Alzheimer’s disease).
Memantine hydrochloride is an adamantine derivative. The patent was granted on 15 September 1993 and expired on 13 April 2009
(‘the basic patent’). According to the order for reference, the patent was granted despite the earlier commercial availability
of memantine because it concerned a second medical use of memantine.

26.      On 15 May 2002, the European Medicines Agency (EMA) granted H Lundbeck A/S, the licensee of Merz, a series of marketing authorisations,
valid within Community territory, for the product memantine hydrochloride and the drug Ebixa, designed for the treatment of
Alzheimer’s disease (collectively designated: ‘the 2002 marketing authorisation’). The German and Luxembourg marketing authorisations
were, consequently, revoked.

27.      On 13 November 2002, Merz applied to the United Kingdom Patent Office for an SPC, citing the basic patent and the 2002 marketing
authorisation. The SPC was obtained on 14 August 2003 for a period of five years as of the expiry of the basic patent (‘the
Merz SPC’ or the ‘SPC at issue’). It therefore took effect as of 14 April 2009 and will expire on 13 April 2014.

28.      Synthon, a manufacturer of generic drugs, brought an action before the High Court of Justice (Chancery Division) Patents Court,
seeking revocation of Merz’s SPC or a declaration that the latter’s term of protection is fixed at zero.

29.      By its action, Synthon claims that the 2002 marketing authorisation is not the first marketing authorisation for memantine
as a medicinal product, for it had already been authorised, in 1983, in Luxembourg, as an ingredient of Akatinol. Merz’s SPC
is, therefore, invalid in that it fails to satisfy the requirements of Article 3 of the regulation or, in the alternative,
is invalid or has zero term, pursuant to Article 13 of the regulation, because the first marketing authorisation in the Community
predates the filing of the patent application. In the further alternative, Synthon claims that the SPC at issue is invalid
because the first marketing authorisation in the Community was obtained before 1 January 1985 in breach of Article 19(1) of
the regulation, or because memantine was marketed as a medicinal product before authorisation was obtained in accordance with
Directive 65/65, in breach of Articles 2 and 3 of the regulation.

30.      In its examination of the case, the national court entertained doubts concerning the proper interpretation of certain provisions
of the regulation and submitted the four following questions for a preliminary ruling;

‘(1)      For the purposes of Articles 13 and 19 of Council Regulation (EC) No 1768/92, is an authorisation a ‘first authorisation to
place ... on the market in the Community’, if it is granted in pursuance of a national law which is compliant with Council
Directive 65/65/EEC, or is it necessary that it be established in addition that, in granting the authorisation in question,
the national authority followed an assessment of data as required by the administrative procedure laid down in that directive?

(2)      For the purposes of Articles 13 and 19 of Council Regulation (EC) No 1768/92, does the expression ‘first authorisation to
place ... on the market in the Community’ include authorisations which had been permitted by national law to co-exist with
an authorisation regime which complies with Council Directive 65/65/EEC?

(3)      Is a product which is authorised to be placed on the market for the first time in the EEC without going through the administrative
procedure laid down in Council Directive 65/65/EEC within the scope of Council Regulation (EC) 1768/92 as defined by Article
2?

(4)      If not, is an SPC granted in respect of such a product invalid?’

III –  **Procedure before the Court**

31.      Synthon, Merz and the Commission submitted written observations pursuant to Article 23 of the Statute of the Court of Justice
and were heard at the hearing on 9 December 2010.

IV –  **Assessment**

32.      The third and fourth questions, by which the national court seeks to ascertain the substantive scope of the regulation, raise
an issue that needs to be resolved before the points raised by the first and second questions can be settled. I shall therefore
begin my analysis by examining that issue.

A –    *The third and fourth questions*

33.      By its third and fourth questions, the national court, in essence, asks the Court of Justice to clarify whether, on the one
hand, the products for which a marketing authorisation under Directive 65/65 was granted after those products had first been
placed on the market fall within the scope of the regulation, as defined by Article 2 thereof, and, on the other, if this
is not the case, whether an SPC obtained for such products must be deemed to be invalid in accordance with the regulation.

34.      According to Merz, only authorisations obtained in accordance with Directive 65/65 in the Member State in which the SPC application
is made are covered by the regulation. It takes the view that a product placed on the market in the Community for the first
time without adhering to the procedure laid down in the directive, as in the case of memantine, falls within the scope of
the regulation if it is covered by a patent in the Member State in question and if, before being placed on the market in that
Member State, it was subject to an administrative authorisation procedure pursuant to Directive 65/65. However, Synthon and
the national court are of the view that memantine does not fall within the scope of the regulation, for it was marketed in
the Community before a marketing authorisation consistent with Directive 65/65 was obtained.

35.      Under Article 2 of the regulation, ‘[a]ny product protected by a patent in the territory of a Member State and subject, prior
to being placed on the market as a medicinal product, to an administrative authorisation procedure as laid down in Council
Directive 65/65/EEC’ may be the subject of a certificate.

36.      The Court is asked, in essence, to clarify whether, as Merz contends, Article 2 refers to the placing on the market *in the Member State* in which the SPC application was made or, as Synthon argues, to the first placing on the market *in the territory of the Community*. ([13](#Footnote13))

37.      Opting for either one or the other of the interpretations advanced on the basis of literal and/or systematic arguments does
not appear to be easy, given that, as the parties to the main proceedings and the national court itself have pointed out,
there are factors that argue for one interpretation and others that argue for the contrary interpretation.

38.      In particular, it is certainly true, as Merz submits, that Article 2 refers to products covered by a patent in a Member State,
and that it would, therefore, be logical to conclude that, when Article 2 refers to the placing of the product on the market,
this must be construed as referring to the territory of that Member State. More generally, that interpretation would be consistent
with the establishment of the SPC as a national intellectual property right.

39.      However, it is also true that, if the expression ‘placing on the market’ were interpreted as Merz seeks to construe it, Article
2 would end up pointlessly duplicating Article 3, while it would seem logical to construe Article 2 as a provision defining
the scope of the regulation, restricting it to ‘new medicinal products’, ([14](#Footnote14)) that is to say, products which have been subject to a procedure under Directive 65/65 before being placed on the market in
Community territory, and to interpret Article 3 as a provision laying down the conditions for obtaining an SPC.

40.      In those circumstances, therefore, it is on the basis of the objectives of the regulation that the question referred for an
interpretation by the High Court must be resolved.

41.      As is evident from the preamble to the regulation (and recitals 2, 3 and 4 in particular), the purpose of the regulation is
to limit the extent to which the duration of the exclusive right is eroded as a result of the implementation of the administrative
authorisation procedure which, by delaying the placing of the product on the market, defers the point at which the patent
can begin to be commercially exploited. In that way, the Community legislature sought to provide the Community pharmaceutical
industry with a means of securing an adequate economic return on the investment needed for research, and to enable it to bridge
the competitive gap with non-member countries.

42.      At the same time, the regulatory scheme of the regulation is clearly based on striking a balance between the conflicting interests
of, on the one hand, the pharmaceutical manufacturers and their licensees and, on the other, the generic medicines industry
that stimulates price competition in the pharmaceuticals sector. Striking that balance has resulted in the imposition of a
maximum time-limit on the exclusive right of exploitation guaranteed by the combination of patent and SPC – a time-limit which
is, moreover, set at a level lower than is accorded under the patent (15 rather than 20 years).

43.      The Court’s case-law displays a tendency to adhere to the system based on that balance of interests. For instance, on the
one hand, it protects the whole function of the regulation as an instrument for protecting the pharmaceuticals industry which
relies on research, by guaranteeing the effectiveness of that research, ([15](#Footnote15)) and, on the other, it ensures that such protection does not go beyond the objectives pursued by the regulation itself. ([16](#Footnote16))

44.      Moreover, the regulation is designed to provide a uniform solution at Community level to the problem of the inadequacy of
the protection under patent and thus prevent the heterogeneous development of national laws. As emphasised by Advocate General
Jacobs, ‘[t]hat uniformity [is] probably the most significant result of the certificate introduced by the regulation’. ([17](#Footnote17))

45.      It is in the light of all of the factors set out in the preceding points that I tend towards the argument set out by Synthon.
I do not, in fact, consider it compatible with the objectives of the regulation to extend the protection provided under the
SPC to products which were already present on the Community market on a different basis before the marketing authorisation
was obtained in accordance with Directive 65/65. ([18](#Footnote18))

46.      On the one hand, it does not appear justified to confer that protection on products which, although covered by a patent in
the Member State in which the certificate was applied for, and although marketed in that State only after having obtained
marketing authorisation in accordance with the relevant Community legislation, were already on the market, in another part
of Community territory, on a different basis and without the tests required under Community law having been carried out. The
fact that, at the time when they were first placed on the market, those products may not have been covered by an exclusive
marketing right is immaterial in that regard. ([19](#Footnote19))

47.      On the other hand, if, in such cases, the protection afforded by the regulation were recognised, then the period of exclusive
commercial exploitation of a patent-protected product, beginning when that product is first placed on the Community market,
could, in certain specific cases, exceed the 20-year period of the patent’s validity.

48.      I do not consider that any other solution can be justified solely in view of the national character of the SPC. In point of
fact, while there is no doubt that the regulation is designed to establish an intellectual property right of national character,
one of its principal objectives remains, as we have seen, to ensure the uniformity of the rules on certificates issued within
the territory of the Union, in particular as regards their duration and the overall extent in time of the guarantee of exclusivity.
Were Merz’s argument to be adopted, that objective would be undermined, not only for the reasons set out above, but also because
that argument implies that, for one and the same product, it would be possible to obtain a certificate in some Member States
(those in which a marketing authorisation was obtained in accordance with the Community law before the product was placed
on the market in that State), but not in others (States in which the product had already been marketed earlier on a different
basis).

49.      Furthermore, the interpretation which Merz suggests would create an unjustified disparity of treatment in relation to products
placed on the market before the date fixed by Article 19 of the regulation. In effect, for products for which marketing authorisation
in accordance with Directive 65/65 was obtained before that date, the possibility of applying for an SPC would be precluded
by that provision. However, the same would not apply to products placed on the market, before the date set by Article 19 of
the regulation, on a different basis and for which marketing authorisation pursuant to Directive 65/65 was not obtained until
after that date.

50.      On the basis of the foregoing, I consider that, in accordance with Article 2 thereof, the regulation must be interpreted as
meaning that products placed on the market as medicinal products in Community territory before a marketing authorisation in
accordance with the relevant Community legislation has been obtained do not fall within the scope of the regulation. Having
been obtained for a product which does not fall within the scope of the regulation, the SPC at issue in the main proceedings
must be regarded as invalid. That finding flows from the interpretation of Article 2 proposed above, and it does not seem
to me that Article 15 of the regulation, which lists the reasons why an SPC may be invalid, stands in its way.

51.      In the light of the answers which I propose be given to the third and fourth questions, it is solely in the alternative, should
the Court not agree with that solution, that I shall go on to assess the first and second questions.

B –    *The first and second questions*

52.      By its first and second questions, which it is appropriate to examine together, the national court asks, in essence, both
whether a marketing authorisation obtained without the tests required under Article 4(8) of Directive 65/65 having been carried
out may constitute a first marketing authorisation in the Community, for the purpose of Articles 13 and 19 of the regulation
and, also, whether a marketing authorisation which is permitted, under the national law transposing the directive, to co-exist
with a system of authorisation consistent with the directive may also constitute a first marketing authorisation. ([20](#Footnote20))

53.      Article 13 of the regulation lays down the procedures for calculating the term of the SPC in such a way as to harmonise the
date of expiry of the various national SPCs obtained in the territory of the Union. So, while, as Merz correctly points out,
it is the first marketing authorisation obtained in the requested Member State which counts for the purposes of submitting
the SPC application, when, on the other hand, it comes to calculating the term of the SPC, the marketing authorisation to
be taken into consideration is the first marketing authorisation obtained in the Community. This may be the first marketing
authorisation obtained in the requested Member State, but it can also be a marketing authorisation obtained earlier.

54.      In this case, Merz maintains that the first marketing authorisation in the Community for the purpose of Article 13 is the
2002 marketing authorisation, for it was the first marketing authorisation for memantine that satisfied the substantive requirements
of Directive 65/65. Synthon, however, contends that either the German marketing authorisation or the Luxembourg authorisation
should be regarded as the first marketing authorisation in the Community, despite the fact that neither was obtained after
completion of the tests required under the directive.

55.      The Court has already had occasion to interpret the concept of ‘first authorisation to place on the market’ in its judgments
in *Hässle* ([21](#Footnote21)) and *Novartis*, ([22](#Footnote22)) which are cited by both parties in the main proceedings, although with contrary arguments.

56.      In *Hässle*, the Court held that an authorisation provided for under a national law on the pricing of medicinal products, which must
be obtained before those products can actually be marketed, cannot constitute a ‘first authorisation to place on the market’
pursuant to Article 19 of the regulation.

57.      In *Novartis*, however, the Court found that the concept of ‘first authorisation to place on the market’ under Article 13 of the regulation,
as it has to be construed for the purposes of interpreting the Agreement on the European Economic Area (‘EEA Agreement’),
includes a marketing authorisation granted by the Swiss authorities and automatically recognised by the Principality of Liechtenstein
in the context of its regional union with Switzerland.

58.      As the national court points out, neither of the solutions adopted by the Court in those judgments can automatically be transposed
to this case.

59.      Indeed, on the one hand, in *Hässle*, the Court was dealing with a national authorisation which was, by its very nature, different from a marketing authorisation
under Directive 65/65, although comparable to such an authorisation in terms of the effects on the possibility of marketing
the product. On the other hand, the interpretation of Article 13 of the regulation in *Novartis* is specifically restricted to the context of the application of the EEA Agreement.

60.      Nonetheless, both precedents provide important interpretative guidance

61.      In *Hässle*, the Court found, and did not mince its words, that ‘[t]here is thus nothing to justify the words “authorisation to place
... on the market” being interpreted differently depending on which provision of Regulation [No 1768/92] they appear in’ and
that ‘those words cannot be construed as having a different meaning according to whether they appear in Article 3 or Article 19’. ([23](#Footnote23)) Synthon’s argument that different significance should be attributed to the concept of a marketing authorisation for the purposes
of calculating the term of the SPC does not, therefore, appear to be tenable. The Court has in fact found unequivocally in
favour of a uniform interpretation of that concept, wherever it appears in the regulation.

62.      In the same judgment, and equally unambiguously, after stating that ‘neither Article 19 of Regulation No 1768/92, nor any
other provision of that regulation, nor the recitals therein mentions, whether expressly or by implication, any authorisation
other than that relating to provisions on medicinal products in accordance with Directive 65/65’, the Court concluded that
the ‘“first authorisation to place ... on the market ... in the Community”, mentioned in, among others, Article 19(1) of Regulation
[No 1768/92], must ... be a marketing authorisation issued in accordance with Directive 65/65’. ([24](#Footnote24))

63.      The Court thus opted for a formalistic approach – founded on what are essentially reasons bound up with the need for legal
certainty ([25](#Footnote25)) – which differs from an approach that focuses to a greater degree on the objectives of the regulation, as set out in his
Opinion in *Novartis* by Advocate General Ruiz Jarabo-Colomer. According to the approach taken by the latter, for the purposes of calculating the
term of the SPC, the concept of ‘first authorisation to place on the market in the Community’ should extend to any measure
which makes possible the lawful distribution of a medicinal product in a part of the Union’s territory. ([26](#Footnote26))

64.      In its judgment in *Novarti*s, albeit in a specific context, the Court appears to have moderated the formalistic approach which it adopted in its judgment
in *Hässle*. Without ever citing the latter judgment, the Court still included in the concept of first marketing authorisation in the
EEA, in accordance with Article 13 of the regulation, a Swiss authorisation which was automatically recognised in the Principality
of Liechtenstein and, therefore, clearly not consistent with Directive 65/65. At paragraphs 29 and 30 of the judgment, the
Court’s reasoning in reaching that finding is linear: since the EEA Agreement recognises that two types of marketing authorisation
may co-exist in the Principality of Liechtenstein, namely marketing authorisations issued by the Swiss authorities which,
because of the regional union between Switzerland and Liechtenstein, are automatically recognised in Liechtenstein, and marketing
authorisations issued in Liechtenstein in accordance with Directive 65/65, the former, like the latter, must be taken into
consideration for the purposes of applying Article 13 of the regulation. ([27](#Footnote27))

65.      The High Court is not, however, of the view that the guidance which may be derived from the judgment in *Novartis* is sufficient to justify moving away from the Court’s position in *Hässle*. Moreover, in a judgment handed down in the context of a dispute which arose in relation to an SPC application for memantine
by Merz, in Germany, the German Patentgericht (Patent Court) took the view that the Court’s position in its judgment in *Hässle* meant that neither the German market authorisation nor the Luxembourg market authorisation could be recognised as the first
authorisation to place the product on the market in accordance with Article 13 of the regulation. ([28](#Footnote28))

66.      It is necessary, at this juncture, to look in greater detail at the marketing authorisation in question.

67.      It is not disputed that neither the German marketing authorisation, obtained by Merz following notification in accordance
with Article 3(7) of the AMG 1976, nor the Luxembourg marketing authorisation, granted on the basis of the earlier German
authorisation, was issued on the basis of dossiers containing the results of the toxicological and pharmacological tests and
clinical trials required at the time under Directive 65/65. ([29](#Footnote29)) Nor is it disputed that those results were not provided at a later date during the period of validity of those marketing
authorisations.

68.      Both marketing authorisations were adopted under the respective national laws transposing Directive 65/65, but there are significant
differences.

69.      The German authorisation was granted in accordance with transitional arrangements, provided for under the national legislation
transposing Directive 65/65, which exempted medicinal products already on the market from the application of the Community
authorisation procedure for a period of 12 years as of 1 January 1978, provided that the competent authorities were notified.
Those arrangements implemented Article 24 of that directive, in conjunction with Article 39 of Directive 75/319, and as amended
by Article 37 of the latter, ([30](#Footnote30)) which made it possible progressively to apply ([31](#Footnote31)) the provisions of Directive 65/65 to medicinal products placed on the market before the directive’s entry into force and,
consequently, permitted, on a transitional basis, the circulation of medicinal products on which the requisite tests had not
been carried out, as in the case of Akatinol.

70.      The Luxembourg marketing authorisation, however, was granted solely on account of the fact that Akatinol was lawfully marketed
in Germany on the basis of a so-called ‘fictitious’ authorisation (‘fiktive Zulassung’). ([32](#Footnote32)) Unlike the German authorisation, the Luxembourg authorisation was not, therefore, issued on the basis of national transitional
arrangements implementing Article 24 of Directive 65/65.

71.      Consequently, in order to answer the first and second questions, it is necessary to clarify whether a marketing authorisation
with the features described above can be regarded as having been ‘issued in accordance with Directive 65/65’ within the meaning
of the judgment in *Hässle* and can, therefore constitute a first authorisation to place on the market in the Community for the purposes of calculating
the term of the SPC in accordance with Article 13, as well as for the purposes of the application of Article 19.

72.      Pursuing the line of reasoning employed by the national court when drawing up the first and second questions, it is necessary
to begin by considering whether a marketing authorisation which, although issued in accordance with the national legislation
transposing Directive 65/65, did not comply with the administrative procedure laid down by the directive, may constitute a
first marketing authorisation in accordance with Articles 13 and 19 of the regulation.

73.      In my view, a marketing authorisation issued *pursuant to* the provisions transposing Directive 65/65 must certainly be regarded, where appropriate, as the ‘first authorisation to
place on the market in the Community’, even if the administrative procedure laid down under the directive has not, in fact,
been implemented or has not been properly implemented, particularly as regards the toxicological and pharmacological tests
and clinical trials.

74.      Indeed, in a case of that nature, although the marketing authorisation fails to satisfy the substantive requirements of Directive
65/65, it nonetheless fits, from a formal perspective, within the scheme of the directive. In those circumstances, it does
not appear justified to impose on the authorities responsible for granting the SPC the burden of verifying whether the procedure
followed for the purpose of granting a marketing authorisation, accorded on the basis of the national legislation transposing
Directive 65/65, is compatible with the Community legislation. Moreover, the regulation itself does not require such verification.
By requiring that the SPC application must state the number and date of the first authorisation to place the product on the
market in the Community, information regarding the identity of the product, the legal provision under which the authorisation
procedure took place and a copy of the notice publishing the authorisation in the appropriate official publication, Article
8(a)(iv) (b) and (c) of the regulation merely requires verification that the authorisation actually exists, as well as verification
of the identity of the authorised product and, at most, purely formal verification that it was issued under harmonised legislation. ([33](#Footnote33))

75.      In this case, however, the circumstances set out at point 73 above do not appear to be present. While it is true that both
the German and the Luxembourg marketing authorisations were issued *on the basis of* the respective national provisions transposing Directive 65/65, neither may be regarded as having been issued *pursuant to* national provisions transposing the administrative authorisation procedure laid down by the directive. As we in fact saw
earlier, the German marketing authorisation was obtained under the transitional arrangements permitted by Article 24 of the
directive, and the Luxembourg marketing authorisation by virtue of the automatic recognition of the German marketing authorisation,
by means of a mechanism falling outside the system of mutual recognition provided for by the directive, which relates solely
to marketing authorisations issued on completion of the administrative procedure which it lays down.

76.      In those circumstances, the marketing authorisations at issue cannot, in my view, be regarded as being ‘consistent’ with Directive
65/65. In particular, the Commission seems to me to go too far in arguing that in order to secure such compliance for the
purposes of applying the provisions of the regulation, it is sufficient that the marketing authorisation was issued by the
competent authorities of a State in which there is an obligation to refrain from authorising the placing on the market of
medicinal products which have not been subjected to the procedure laid down by the directive. On the basis of that argument,
in fact, it would also be necessary to regard authorisations that may have been issued on the basis of national provisions
which are not those transposing the directive as being consistent with Directive 65/65. ([34](#Footnote34))

77.      Having ruled out the possibility that the German and Luxembourg marketing authorisations obtained by Merz for memantine and
Akatinol can be deemed to be ‘consistent’ with Directive 65/65, it is necessary to consider whether, nonetheless, as Synthon
contends, such authorisations may, none the less, be taken into account in determining which was the first marketing authorisation
in the Community for memantine.

78.      In my view, particularly as regards the German marketing authorisation, the answer must be in the affirmative, based on a
line of reasoning similar to that set out by the Court at paragraphs 29 and 30 of its judgment in *Novartis* which may well extend beyond the specific context of that case.

79.      Since Directive 65/65 permitted, albeit on a transitional basis, the possible co-existence in the Member States of two authorisation
regimes, namely, the regime actually established by the directive and the regime permitted under Article 24 thereof, authorisations
issued on the basis of Article 24 must, if appropriate, be regarded as the first marketing authorisations within the meaning
of Articles 13 and 19 of the regulation. In this case, that would be the German marketing authorisation.

80.      That solution is consistent with the rationale underlying the regulation which, as we have seen, is designed to limit the
extent to which the period of exclusivity under the patent is eroded as a result of the time elapsing between the filing of
the patent application and the completion of the administrative procedure for marketing the product required under Directive
65/65, but without exceeding a 15-year period of exclusive use, which the legislature considered appropriate in order to strike
a balance between the conflicting interests involved. ([35](#Footnote35)) If, when calculating the term of the SPC, account were not taken of the authorisations issued under national arrangements
set in place pursuant to Article 24 of Directive 65/65, it would be possible to retain for far longer marketing exclusivity
for products covered by a patent at the time they were placed on the market. Furthermore, as emphasised by Synthon, the contrary
solution would have the perverse effect of allowing reappraisal of the period of exclusivity under the patent without taking
account of the fact that, as in the case of memantine, it was possible for the product in question to be in circulation under
transitional arrangements without satisfying the requirements of Community law. ([36](#Footnote36)).

81.      In my view, the same solution should also apply in circumstances in which the system selected by the Member State in order
progressively to achieve compliance with the provisions of the directive in relation to medicinal products which have already
been placed on the market, as laid down by Article 24 of Directive 65/65 and Article 39 of Directive 75/319, provides not
for the grant of new authorisations (those described as fictitious or post-marketing authorisations), as in the case of Germany,
but solely for extension of the validity of the original authorisations. ([37](#Footnote37)) In such cases, the reference point for the application of Articles 13 and 19 of Directive 65/65 should be the date on which
that extension first takes effect.

82.      I do not, however, consider that significance need be attached to the period before that extension or the grant of a post-marketing
authorisation. In effect, it is only on the basis of an extension or authorisation of that nature that the circulation of
the medicinal products placed on the market of one Member State, pursuant to provisions which predate the entry into force
of Directive 65/65, may be regarded as lawful under the provisions of that directive, albeit solely on a transitional basis
and subject to subsequent compliance with its requirements (see the conditions laid down in Article 39(2) and (3)) [of Directive
75/319/EEC]. Consequently, I do not consider that the basis on the strength of which a medicinal product of that nature was
originally placed on the market may be regarded as the first marketing authorisation in the Community, even if it does coincide
with the time when the marketing of the product in Community territory was authorised for the first time.

83.      Moreover, a finding of that nature satisfies the requirements of legal certainty to which the Court itself referred in its
judgment in *Hässle*, ([38](#Footnote38)) and also the requirement that the rules on the SPC be uniform and simple to apply, to which particular emphasis was attached
during the legislative process for the adoption of the regulation. Verifying the existence and the date of initial validity
of national authorisations granted prior to the harmonisation brought about by Directive 65/65 may prove to be a complex process,
whereas it is certainly simpler to undertake that verification when it turns on the authorisation based on which medicinal
products already placed on the market may continue to be marketed lawfully under the transitional arrangements set in place
by Directive 65/65.

84.      Before I draw the conclusions from the above analysis, it is necessary to consider a further issue which, although it was
not raised by the national court may, nonetheless, influence the answer to be given to the first and second questions and,
more generally, the solution of the dispute before it.

85.      That issue, on which the parties in the main proceedings had the opportunity to state a view at the hearing, is raised by
the Commission in the context of the request for a preliminary ruling referred by the Court of Appeal in the case of *Generics* v *Synaptech*, which was mentioned earlier, and it concerns the possibility of taking into account, when determining the term of the SPC,
an authorisation issued for a use of the product different from that protected by the basic patent. In essence, relying on
the text of Article 4 of the regulation, the Commission argues that the protection conferred by the SPC covers all of the
uses of the product for which a marketing authorisation has been obtained, provided that those uses are caught by the subject-matter
of the basic patent. According to the Commission, it follows that, for the purposes of applying Articles 13 and 19 of the
regulation, it is not possible to regard as the first marketing authorisation in the Community a marketing authorisation issued
for a product use other than the use or uses covered by the basic patent.

86.      I do not find the Commission’s argument compelling. Article 4 of the regulation defines the *subject-matter of the protection* conferred by the SPC, making it clear both that such protection extends only to the protection conferred by the basic patent
and that the SPC covers any subsequent marketing authorisation in relation to the product’s use as a medicinal product granted
during the term of validity of the SPC, thereby precluding the possibility of obtaining an SPC for each marketing authorisation
for the product obtained in a single Member State.

87.      However, Article 13 of the regulation concerns the *duration* of the SPC and Article 19 introduces transitional provisions laying down certain *conditions governing the issuing of the SPC*. It is apparent from both the wording and scheme of those provisions that the marketing authorisation in the Community to
which they refer is the first marketing authorisation *for the product as a medicinal product*. ([39](#Footnote39)) For the purposes of the application of those articles, no reference is made to a specific therapeutic use, still less to
the use or uses covered by the basic patent, despite the fact that the regulation provides specifically that a basic patent
may cover both a product as such and an application of that product. ([40](#Footnote40))

88.      The regulation therefore justifies an interpretation according to which, for the purposes of the application of Articles 13
and 19, the first marketing authorisation for the product as a medicinal product must be regarded as the first marketing authorisation
in the Community, regardless of the kind of medical use which constitutes the subject-matter of that authorisation and regardless
of whether that use may possibly be the same as the use protected by the basic patent.

89.      That interpretation is, above all, in keeping with the concept of product for the purpose of the regulation, as interpreted
by the Court’s case-law. I would point out, in that connection, that, according to Article 1(b) of the regulation, product
means ‘the active ingredient or combination of active ingredients of a medicinal product’. In its judgment in *Massachusetts Institute of Technology*, the Court provided clarification that the concept of ‘product’, within the meaning of Article 1(b) of the regulation, must
be interpreted in the strict sense of an ‘active substance’ or ‘active ingredient’. ([41](#Footnote41)) Relying on that judgment, in its Order in *Yissum*, the Court explained that the concept of product ‘cannot include the therapeutic use of an active ingredient protected by
a basic patent’ and that ‘Article 1(b) of Regulation No 1768/92 is to be interpreted as meaning that in a case where a basic
patent protects a second medical use of an active ingredient, that use does not form an integral part of the definition of
the product’. ([42](#Footnote42))

90.      Moreover, the interpretation suggested at point 88 above is borne out by a number of the Court’s judgments. In its judgment
in *Pharmacia Italia*, the Court held that ‘the grant of a certificate in a Member State of the Community on the basis of a medicinal product for
human use authorised in that Member State is precluded by a marketing authorisation for that product as a veterinary medicinal
product granted in another Member State of the Community before the date specified in Article 19(1) of the regulation’. ([43](#Footnote43)) At paragraph 20 of that judgment, after recalling, in paragraph 19, the concept of ‘product’ within the meaning of Article
1(b) of the regulation, and also the wording of Articles 3 and 4, the Court stated that ‘the decisive factor for the grant
of the certificate *is not the intended use of the medicinal product*’ and that ‘the protection conferred by the certificate relates to *any use of the product as a medicinal product* without any distinction between use of the product as a medicinal product for human use and as a veterinary medicinal product’. ([44](#Footnote44)) Lastly, in its judgment in *Biogen*, the Court held that when a product is protected by a number of basic patents,([45](#Footnote45)) each of those patents may be designated for the purpose of the procedure for the grant of a certificate, ([46](#Footnote46)) making plain, however, that ‘as is clear from Article 13 of the regulation, the duration of such certificates is to be calculated
uniformly on the basis of the date of the first authorisation to place the product on the market in the Community’. ([47](#Footnote47))

91.      On the basis of what I have set out at points 86 to 90 above, I am of the view that there is nothing to preclude a marketing
authorisation granted for a use of the product different from the use or uses protected by the basic patent from being regarded
as the first marketing authorisation in the Community, for the purposes of the application of Articles 13 and 19 of the regulation.

92.      In the light of all the foregoing considerations, I propose that the Court’s answer to the first and second questions should
be that an authorisation granted by the authorities of a Member State in accordance with the national provisions transposing
Directive 65/65 may constitute the first marketing authorisation in the Community for the purpose of Articles 13 and 19 of
the regulation, even when the administrative procedure for which the directive provides has, in fact, not been implemented
or has not been properly implemented, particularly as regards the carrying out of the toxicological and pharmacological tests
and the clinical trials required by Article 4(8) of the directive and the notification of the results of those tests and trials.

93.      Similarly, a marketing authorisation granted by the competent authorities of a Member State, under the transitional arrangements
provided for by Article 24 of Directive 65/65, in conjunction with Article 39 of Directive 75/319, and as amended by Article
37 of the latter directive, on the basis of a marketing authorisation granted before the transposition of Directive 65/65
into the legal order of that Member State, may be regarded as the first marketing authorisation in the Community within the
meaning of the abovementioned provisions.

94.      Based on the solution which I propose, even supposing that the SPC obtained by Merz was validly granted, ([48](#Footnote48)) the term of that SPC was, in any event, calculated incorrectly inasmuch as the 2002 marketing authorisation was taken into
consideration for the purposes of that calculation, rather than the German authorisation which, on the basis of the foregoing,
must be regarded as the first marketing authorisation in the Community for the purpose of Article 13 of the regulation. Assuming
the German marketing authorisation to be the authorisation of reference, the term of the SPC granted to Merz must be fixed
at zero.

V –  **Conclusions**

95.      On the basis of all of the foregoing considerations, I propose that the Court should give the following answers to the questions
submitted by the High Court of Justice (Chancery Division):

‘Council Regulation (EEC) No 1768/92 of 18 June 1992 concerning the creation of a supplementary protection certificate for
medicinal products, must be interpreted, pursuant to Article 2 thereof, as meaning that products placed on the market as medicinal
products in Community territory before obtaining a marketing authorisation in accordance with Council Directive 65/65/EEC
on the approximation of the provisions laid down by law, regulation or administrative action relating to proprietary medicinal
products or with Council Directive 81/851/EEC of 28 September 1981 on the approximation of the laws of the Member States relating
to veterinary medicinal products do not fall within the scope of the regulation.

Supplementary protection certificates granted for such products must be deemed to be invalid.’

96.      Should the Court not adopt that solution, I propose that it should give the following answers to the first and second questions
submitted by the High Court of Justice (Chancery Division):

‘A marketing authorisation granted by the authorities of a Member State in accordance with the national provisions transposing
Directive 65/65 may constitute the first marketing authorisation in the Community for the purpose of Articles 13 and 19 of
Regulation No 1768/92, even when the administrative procedure for which the directive provides has not been implemented or
has not been properly implemented, particularly as regards the carrying out of the toxicological and pharmacological tests
and the clinical trials required by the directive.

A marketing authorisation granted by the competent authorities of a Member State, under the transitional arrangements provided
for by Article 24 of Directive 65/65, in conjunction with Article 39 of Second Council Directive 75/319/EEC of 20 May 1975
on the approximation of provisions laid down by law, regulation or administrative action relating to proprietary medicinal
products, and as amended by Article 37 of that directive, may also constitute the first marketing authorisation of the product
in the Community, on the basis of a marketing authorisation granted before the transposition of Directive 65/65 into the legal
order of that Member State.

For the purposes of the application of Articles 13 and 19 of Regulation No 1768/92, a marketing authorisation granted for
a use of the product as a medicinal product different from the use or uses protected by the patent constituting the basic
patent under Article 1(c) of that regulation may also be regarded as the first marketing authorisation in the Community’.

---

[1](#Footref1) – Original language: Italian.

---

[2](#Footref2) – Council Regulation (EEC) No 1768/92 concerning the creation of a supplementary protection certificate for medicinal products
(OJ 1992 L 182, p. 1).

---

[3](#Footref3) –      The first certificates of this kind were granted in the United States in 1985, with the Japanese certificates following as
of 1988. In Europe, that form of supplementary protection under patent was first introduced in certain Member States (Italy,
France and Sweden) and subsequently regulated at Community level.

---

[4](#Footref4) – OJ, English Special Edition 1965-1966, p. 20. As of 18 December 2001, Directive 65/65 was replaced by Directive 2001/83/EC
of the European Parliament and of the Council on the Community Code relating to medicinal products for human use (OJ 2001
L 311, p. 67).

---

[5](#Footref5) – Namely the amended version of the Second Council Directive 75/319/EEC of 20 May 1975 on the approximation of provisions
laid down by law, regulation or administrative action relating to proprietary medicinal products (OJ 1975 L 147, p. 13). The
later amendments post-date the marketing of Akatinol in Germany and Luxembourg.

---

[6](#Footref6) – According to Article 1, first subparagraph, (1), for the purposes of the directive, ‘proprietary medicinal product’ meant
‘[a]ny ready-prepared medicinal product placed on the market under a special name and in a special pack’, and medicinal product’
‘[a]ny substance or combination of substances presented for treating or preventing disease in human beings or animals’.

---

[7](#Footref7) – Cited in footnote 5. That directive too was repealed by Directive 2001/83.

---

[8](#Footref8) – It was notified on 3 February 1965.

---

[9](#Footref9) – As of 6 July 2009, Regulation No 1768 was repealed and replaced by Regulation No 469/2009, cited in footnote 2.

---

[10](#Footref10) – Subsequently amended by the Act of Accession of Austria, Finland and Sweden to the European Union (OJ 1994 C 241, p. 21).

---

[11](#Footref11) – In its observations, Merz explains that Akatinol was used in the treatment of Parkinson’s disease and for certain other
applications.

---

[12](#Footref12) – In reality, the first marketing authorisation for Memantine and Akatinol in Germany dates back earlier and was granted
on the basis of legislation from 1961. However, for the purposes of this Opinion, I shall regard the authorisation to keep
Akatinol on the market, which was granted under the AMG 1976, as the German marketing authorisation.

---

[13](#Footref13) – As pointed out by the national court, in the text of the regulation, Article 2 is the only article which contains an ambiguity
of that nature. In all the other provisions, in fact, the Community legislature was careful to specify whether the authorisation
to place on the market had to be construed as relating to the territory of the Member State in which the SPC was applied for
or to the territory of a different Member State (see Article 3(b), Article 8(1)(a)(iv) (b) and (c), Article 9(2)(d) and (e),
Article 11(1)(d) and (e), Article 13(1), Article 19(1) and Article 19a). The Court itself has made a distinction between the
two, emphasising, in its judgment in *Yamanouchi Pharmaceutical*, the different function, within the scheme of the regulation, of the two requirements consisting in the first marketing authorisation
in the Community and the first marketing authorisation in the Member State in which the SPC is applied for (see Case C‑110/95
[1997] ECR I-3251).

---

[14](#Footref14) – See the Proposal for a Council regulation (EEC) concerning the creation of a supplementary protection certificate for medicinal
products (COM (90) 101 final (the ‘Commission’s proposal for a regulation’), paragraph 24.

---

[15](#Footref15) – See Case C-392/97 *Farmitalia* [1997] ECR I-5553, paragraphs 19 and 22, and paragraph 1 of the operative part of the judgment.

---

[16](#Footref16) – See Case C-31/03 *Pharmacia Italia* [2004] ECR I-10001.

---

[17](#Footref17) – See the Opinion of Advocate General Jacobs in *Pharmacia Italia*, cited in footnote 16.

---

[18](#Footref18) – Often not fulfilling the same pharmacological safety requirements.

---

[19](#Footref19) – It does not in fact seem to me that a different conclusion must be reached if, at the time it was placed on the market
as a medicinal product, the product at issue was not covered by a patent. Furthermore, in providing, in Article 13, that the
duration of the certificate is to be calculated as of the date of the first marketing authorisation for the Community, the
regulation itself does not specify that, at the time when the marketing authorisation is granted, the product at issue must
be protected by a patent or be the subject of a patent application (which was not, for example, the case in Case C-258/99
*BASF* [2001] ECR I-3643 concerning a question of the interpretation of Regulation (EC) No 1610/96/EC of the European Parliament
and of the Council concerning the creation of a supplementary protection certificate for plant protection products.

---

[20](#Footref20) – Since the SPC at issue concerns a medicinal product for human use, only Directive 65/65 is relevant in this case.

---

[21](#Footref21) – Case C-127/00 *Hässle* [2003] ECR I-14781.

---

[22](#Footref22) – Joined Cases C-207/03 and C-252/03 *Novartis and Others* [2005] ECR I-3209.

---

[23](#Footref23) – See also *Pharmacia Italia* (cited in footnote 16), paragraph 16.

---

[24](#Footref24) – Paragraphs 56-58.

---

[25](#Footref25) – See paragraph 60.

---

[26](#Footref26) – See point 49 of the Opinion.

---

[27](#Footref27) – Paragraphs 29 and 30.

---

[28](#Footref28) – A similar position was, moreover, adopted, at first instance, by the national court hearing this case, in the context of
a different dispute which gave rise, on appeal, to the reference for a preliminary ruling forming the subject-matter of Case
C-427/09 *Generics (UK)*, on which I am today delivering my Opinion.

---

[29](#Footref29) – The purpose of the requirement that applicants for a marketing authorisation for a medicinal product must attach to the
application the results of the toxicological and pharmacological tests and the clinical trials under Article 8(3)(i) of Directive
2001/83 (formerly required by Article 4 of Directive 65/65) is to provide evidence that a medicinal product is safe and efficacious.
See, to that effect, Case C-440/93 *Scotia Pharmaceuticals* [1995] ECR I-2851, paragraph 17, as well as Case C-368/96 *Generics (UK) and Others* [1998] ECR I-7967, paragraph 23, and Case C-527/07 *Generics (UK)* [2009] ECR I-5259, paragraph 22.

---

[30](#Footref30) – Merz considers that the transitional arrangements under Article 3(7) of the AMG 1976 were not in accordance with Article
24 of the directive. In that connection, it submits, attached to its observations, a Reasoned Opinion of the Commission addressed
to the German Government, by which the Commission disputes the compatibility with the directive of the system of implicit
authorisation provided initially by Article 3(7) of the AMG 1976 and, subsequently, by Article 105 of the amended version
of the AMG. It is, however, clear from reading that document that the criticisms are related solely to the possibility of
marketing products not subjected to the requisite tests *after* the expiry of the transitional stage, that is to say after 21 May 1990.

---

[31](#Footref31) – For 15 years from the date of the notification of Directive 75/319 (which took place on 21 May 1975), according to Article
39 of that directive.

---

[32](#Footref32) – See the letter of 3 July 2009 of the Luxembourg Minister of Health, attached to Merz’ observations. According to that letter,
the Luxembourg authorities too were expecting the documentation on the pharmacological and toxicological tests and the clinical
trials to be completed during the transitional period, but that documentation never materialised.

---

[33](#Footref33) – The purpose of the regulation is to establish a ‘simple transparent’ system for granting SPCs. The Commission’s proposal
for a regulation emphasises, at paragraph 16 that ‘the patents offices should be able to implement the procedure for granting
the certificate without an excessive burden being placed on their administrations’ and that ‘examination of the conditions
to be fulfilled for the certificate to be granted involves the use of objective data that are easy to verify’, as well as
that ‘the adoption of a standard system to calculate the duration of the protection given by the certificate ... means that
the calculation is easy to make’.

---

[34](#Footref34) – I would point out that in Case C-427/09 *Generics (UK)*, on which I am today delivering my Opinion, the Commission has substantially changed the stance it adopted during the written
procedure in this case.

---

[35](#Footref35) – See paragraph 24 of the Commission’s proposal for a regulation.

---

[36](#Footref36) – Moreover, in this case, the German and Luxembourg authorisations were never made consistent with the requirements of Directive
65/65, despite the expiry of the time-limit laid down for that purpose by the directive. Consequently, as far as it is possible
to determine, memantine was able to remain on the market after that that time-limit had expired and in breach of the directive,
until the 2002 marketing authorisations were granted.

---

[37](#Footref37) – As, for instance, in the case of Luxembourg under Article 22 of the abovementioned law of 11 April 1983.

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[38](#Footref38) – Paragraph 60.

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[39](#Footref39) – See Article 19 of the regulation, as well as Article 13, read in the light of Article 3(d) of the regulation.

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[40](#Footref40) – See Article 1(c) of the regulation.

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[41](#Footref41) – Case C-431/04 *Massachusetts Institute of Technology* [2004] ECR I-4089, paragraph 21. At paragraph 19 of the judgment, the Court drew attention to point 11 of the Explanatory
Memorandum to the Proposal for a Council Regulation (EEC), of 11 April 1990, concerning the creation of a supplementary protection
certificate for medicinal products (COM(90) 101 final), stating that ‘(...)[t]he proposal for a regulation therefore concerns
only new medicinal products. It does not involve granting an [SPC] for all medicinal products that are authorised to be placed
on the market. Only one [SPC] may be granted for any one product, a product being understood to mean an active substance in
the strict sense. Minor changes to the medicinal product such as a new dose, the use of a different salt or ester or a different
pharmaceutical form will not lead to the issue of a new [SPC].’

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[42](#Footref42) – Case C-202/05 *Yissum* [2007] ECR I-2839, paragraphs 18 and 20.

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[43](#Footref43) – Cited in footnote 16, paragraph 23.

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[44](#Footref44) – Emphasis added.

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[45](#Footref45) – Case C-181/95 *Biogen* [1997] ECR I-357. The dispute in the main proceedings concerned patents held by a number of owners, but the Court’s reasoning
may also be applied to the situation of patents which protect the product for different therapeutic uses.

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[46](#Footref46) – On condition, according to the Court, that, in accordance with Article 3(c) of the regulation, only one SPC is granted
for each patent.

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[47](#Footref47) – Paragraph 29.

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[48](#Footref48) – Apart from the invalidity that would result were the Court to adopt the answer I have proposed to the third and fourth
questions, it is not clear whether, in this case, the conditions for the application of Article 19(1) of the regulation have
been met. It is not actually apparent from the case-file whether, on the date the regulation entered into force, memantine
was protected by a patent in force, as Article 19(1) requires. If Article 19(1) were applicable, Merz’ SPC would be invalid
because the German marketing authorisation, which was the first marketing authorisation in the Community, dates from before
1 January 1985 and, in any event, because it was applied for after the time-limit of six months from the date of the regulation’s
entry into force, laid down by Article 19(2).

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