# EDGAR Filing Document

**Accession Number:** 0000872912
**File Stem:** 0001193125-23-080977
**Filing Date:** 2023-3
**Character Count:** 46532
**Document Hash:** 50bff74c839bf5410bd3bc2923465e8d
**Contains OCR:** False
**Source Format:** 

## Filing Content

## Filing Summary
**0001193125-23-080977.hdr.sgml**: 20230328

**ACCESSION NUMBER**: 0001193125-23-080977

**CONFORMED SUBMISSION TYPE**: 8-K

**PUBLIC DOCUMENT COUNT**: 55

**CONFORMED PERIOD OF REPORT**: 20230327

**ITEM INFORMATION**: Regulation FD Disclosure

**ITEM INFORMATION**: Financial Statements and Exhibits

**FILED AS OF DATE**: 20230328

**DATE AS OF CHANGE**: 20230327

**FILER**: 

**COMPANY DATA:**
- **COMPANY CONFORMED NAME:** DELCATH SYSTEMS, INC.
- **CENTRAL INDEX KEY:** 0000872912
- **STANDARD INDUSTRIAL CLASSIFICATION:** SURGICAL & MEDICAL INSTRUMENTS & APPARATUS [3841]
- **IRS NUMBER:** 061245881
- **STATE OF INCORPORATION:** DE
- **FISCAL YEAR END:** 1231

**FILING VALUES:**
- **FORM TYPE:** 8-K
- **SEC ACT:** 1934 Act
- **SEC FILE NUMBER:** 001-16133
- **FILM NUMBER:** 23765985

**BUSINESS ADDRESS:**
- **STREET 1:** 1633 BROADWAY
- **STREET 2:** SUITE 22C
- **CITY:** NEW YORK
- **STATE:** NY
- **ZIP:** 10019
- **BUSINESS PHONE:** (212) 489-2100

**MAIL ADDRESS:**
- **STREET 1:** 1633 BROADWAY
- **STREET 2:** SUITE 22C
- **CITY:** NEW YORK
- **STATE:** NY
- **ZIP:** 10019

**FORMER COMPANY:**
- **FORMER CONFORMED NAME:** DELCATH SYSTEMS INC
- **DATE OF NAME CHANGE:** 19990607

?xml version="1.0" encoding="utf-8" ? 8-K

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### UNITED STATES

### SECURITIES AND EXCHANGE COMMISSION

#### Washington, DC 20549

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### FORM 8-K

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#### CURRENT REPORT

#### Pursuant to Section 13 or 15(d)

#### of the Securities Exchange Act of 1934

#### Date of Report (Date of earliest event reported): March 27, 2023

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## DELCATH SYSTEMS, INC.

#### (Exact Name of Registrant as Specified in its Charter)

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| | | |
|:---|:---|:---|
| **Delaware** | **001-16133** | **06-1245881** |
| **(State or other jurisdiction**<br> **of incorporation)** | **(Commission**<br> **File Number)** | **(IRS Employer**<br> **Identification No.)** |

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#### 1633 Broadway, Suite 22C, New York, New York 10019

#### (Address of principal executive offices) (Zip Code)
(212) 489-2100

#### (Registrant's telephone number, including area code)

#### Not Applicable

#### (Former name or former address, if changed since last report)

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Check the appropriate box below if the Form 8-K filing is intended to simultaneously satisfy the filing obligation of the registrant under any of the following provisions:

☐ Written communications pursuant to Rule 425 under the Securities Act (17 CFR 230.425)

☐ Soliciting material pursuant to Rule 14a-12 under the Exchange Act (17 CFR 240.14a-12)

☐ Pre-commencement communications pursuant to Rule 14d-2(b) under the Exchange Act (17 CFR 240.14d-2(b))

☐ Pre-commencement communications pursuant to Rule 13e-4(c) under the Exchange Act (17 CFR 240.13e-4(c))

Securities registered pursuant to Section 12(b) of the Act:

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| | | |
|:---|:---|:---|
| **Title of each class** | **Trading**<br> **symbol(s)** | **Name of each exchange**<br> **on which registered** |
| Common Stock, $.01 par value | DCTH | The Nasdaq Capital Market |

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Indicate by check mark whether the registrant is an emerging growth company as defined in Rule 405 of the Securities Act of 1933 (17 CFR §230.405) or Rule 12b-2 of the Securities Exchange Act of 1934 (17 CFR §240.12b-2).

Emerging growth company ☐

If an emerging growth company, indicate by check mark if the registrant has elected not to use the extended transition period for complying with any new or revised financial accounting standards provided pursuant to Section 13(a) of the Exchange Act. ☐

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| | |
|:---|:---|
| **Item 7.01** | **Regulation FD Disclosure.**  |

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On March 27, 2023, Delcath Systems, Inc. (the "Company") updated its corporate presentation. A copy of the slides used in the presentation are attached hereto as Exhibit 99.1. The furnishing of the attached corporate presentation is not an admission as to the materiality of any information therein. The information contained in the slides is summary information that is intended to be considered in the context of more complete information included in the Company's filings with the U.S. Securities and Exchange Commission (the "SEC") and other public announcements that the Company has made and may make from time to time by press release or otherwise. The Company undertakes no duty or obligation to update or revise the information contained in this report, although it may do so from time to time as its management believes is appropriate. Any such updating may be made through the filing of other reports or documents with the SEC, through press releases or through other public disclosures. For important information about forward looking statements, see the slide titled "Forward Looking Statements" in Exhibit 99.1 attached hereto.

The information in this Item 7.01 of this Current Report on Form 8-K and Exhibit 99.1 attached hereto shall not be deemed "filed" for purposes of Section 18 of the Securities Exchange Act of 1934, as amended, or otherwise subject to the liabilities of that section or Sections 11 and 12(a)(2) of the Securities Act of 1933, as amended. The information contained in this Item 7.01 and in the presentation attached as Exhibit 99.1 to this Current Report shall not be incorporated by reference into any filing with the SEC made by the Company, whether made before or after the date hereof, regardless of any general incorporation language in such filing.

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| | |
|:---|:---|
| **Item 9.01.** | **Financial Statements and Exhibits.**  |

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(d) Exhibits:

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| | |
|:---|:---|
| 99.1 | [Delcath Systems, Inc. Corporate Presentation Dated March 27, 2023](d422467dex991.htm) |
| 104 | Cover Page Interactive File (the cover page tags embedded within the Inline XBRL document) |

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#### SIGNATURE
Pursuant to the requirements of the Securities Exchange Act of 1934, the Registrant has duly caused this report to be signed on its behalf by the undersigned thereunto duly authorized.

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| | | |
|:---|:---|:---|
|  | DELCATH SYSTEMS, INC. | DELCATH SYSTEMS, INC. |
| Date: March 27, 2023 | By: | /s/ David Hoffman |
|  | Name: | David Hoffman |
|  | Title: | General Counsel |

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## Exhibit 99.1

![](g422467ex99_1p1g1.jpg)

Exhibit 99.1 Corporate Presentation (NASDAQ: DCTH) March 26, 2023

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![](g422467ex99_1p2g1.jpg)

Forward-looking Statements The Private Securities Litigation Reform Act of 1995 provides a safe harbor for forward-looking statements made by the Company or on its behalf. This news release contains forward-looking statements, which are subject to certain risks and uncertainties that can cause actual results to differ materially from those described. Factors that may cause such differences include, but are not limited to, uncertainties relating to: actions by the FDA relating to the application; the ability of the Company to respond to FDA queries related to the application; the Company's successful inspections by the FDA or foreign regulatory agencies; the timing and results of the Company's clinical trials, our determination whether to continue a clinical trial program or to focus on other alternative indications, and the impact of the COVID-19 pandemic on the completion of our clinical trials; the impact of the presentations at major medical conferences and future clinical results consistent with the data presented; the Company's ability to successfully commercialize the HEPZATO and the potential of the HEPZATO KIT/CHEMOSAT system as a treatment for patients with primary and metastatic disease in the liver; our ability to obtain reimbursement for commercialized product in various markets; the Company's ability to successfully enter into strategic partnership and distribution arrangements and the timing and revenue, if any, of the same; uncertainties relating to the timing and results of research and development projects; and uncertainties regarding the Company's ability to obtain financial and other resources for any research, development, clinical trials and commercialization activities. These factors, and others, are discussed from time to time in our filings with the Securities and Exchange Commission. You should not place undue reliance on these forward-looking statements, which speak only as of the date they are made. We undertake no obligation to publicly update or revise these forward-looking statements to reflect events or circumstances after the date they are made. 1

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![](g422467ex99_1p3g1.jpg)

Executive Summary Delcath aims to be the leader in targeted, safe and highly-effective minimally-invasive treatments for patients with cancers of the liver. UNMET NEED HEPATIC DELIVERY COMPANY & LARGE MARKET CLINICAL PROGRAM LIVER CANCER SYSTEM (HDS) OPPORTUNITY Incidence US/EU HDS + Melphalan enables FOCUS pivotal trial Near-term (mOM) • Metastatic Ocular • >200K primary and the Percutaneous Hepatic • >$600 TAM in US/EU metastatic liver tumors Perfusion (PHP) Procedure Melanoma (mOM) • Unsurpassed 1 year 1-14 • Primary endpoint met per year • Delivers high dose survival data chemotherapy to the • NDA resubmitted Current local/regional entire liver Longer Term (CRC, ICC, Real World Evidence treatments • Limits systemic exposure Pancreatic, etc.) • Cannot treat the whole • Minimally invasive, • >1k commercial • >>$1B TAM treatments in EU liver repeatable and well- • Investigator interest in • Targeted to visible and tolerated • Multiple single center more than 10 other accessible tumors publications tumor types • Limited in their ability to US: HEPZATO KIT retreat (Melphalan/HDS) EU: CHEMOSAT (HDS) PDUFA Date: 8/14/23 2

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![](g422467ex99_1p4g1.jpg)

Liver-Dominant Cancers High incidence with poor prognosis US Incidence Incid Incid US Incidence ence ence of of of Liv Liv of Liv er er Liv er Dom Dom er Dom Dom inan inan inan inan t t Cancers Cancers t t Cancers Cancers\* (p (p(p a arti rti a(p rti a alla a s s rti l e e sa t t els s t s h h s e o o h t w w o sw n n h))n o) wn) Up to Many patients with liver metastases are 50,000 DELCATH OPPORTUNITY+ not amenable to surgical resection 80% 15 largely due to extensive tumor burden 40,000 30,000 Liver: Common Site of Metastases 20,000 Limited Effective Systemic Treatments » Systemic therapies - low efficacy » Immuno-oncology agents - become less effective in 10,000 the presence of metastases 0 Limited Overall Survival – mOM ICC mBC mNET mPC mCRC HCC Unresectable Liver Cancer » Often the life-limiting organ 1,2 3,4 7-10 \*Metastatic Ocular Melanoma (mOM) , Cholangiocarcinoma (ICC) , Liver-dominant Breast Cancer (mBC) , Metastatic Neuroendocrine 3 6,7 7,13 11,12 15 Tumors (mNET) Metastatic Pancreatic Cancer (mPC) , Metastatic Colorectal Cancer (mCRC) , Hepatocellular carcinoma (HCC) U U.S. .S. In Inc cid ide en nc ce e

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![](g422467ex99_1p5g1.jpg)

Limitations of Current Liver-Directed Therapies 17 16 Trans Arterial Chemo Embolization (TACE) Y90 » Beads obstruct blood flow to tumor and elute chemo » Radioactive beads delivered into the tumor » 50-60k treatments per year in US (and growing) » 10-15k treatments per year in US (and growing) Effective, but tumors Diffuse disease: Many tumors are not recur & retreatment cannot be treated imageable – limited due to with a tumor-by- micro-metastases damaged vasculature tumor modality are common 4 Majority of Treatment

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![](g422467ex99_1p6g1.jpg)

HEPZATO™ Kit: Enables Percutaneous Hepatic Perfusion (PHP) Repeatable, safe & effective liver-focused disease control ISOLATION Hepatic venous flow is isolated, Blood Return Catheter enabling 12x increased dose Chemo Chemo Isolation Filtration (Balloon) Catheter SATURATION Liver Melphalan (chemo) treats micro and macro lesions simultaneously Chemo Delivery Catheter Veno-veno Bypass Pump FILTRATION Proprietary filters remove greater 33 than 85% of chemo from the body 5

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![](g422467ex99_1p7g1.jpg)

mOM: Beachhead Market Opportunity High Unmet Need, Favorable Reimbursement Environment Unmet Need Low Risk Opportunity » >5,000 cases of primary ocular melanoma per year » FOCUS pivotal trial has met primary endpoints to 12,34 2,35 37 in the US/EU , ~50% metastasize to the liver support approval in mOM » US TAM ~800 patients, Europe ~1,200 patients » Significantly improved safety profile over Gen 1 36 filter technology » Median survival up to 12 months. » Real world safety and efficacy demonstrated in EU » 55% of patients have no approved treatment option, most patients treated with multiple lines of therapy High Barrier to Entry Favorable US Commercial Economics » Orphan indication status allows for extended » Favorable US reimbursement environment for ultra exclusivity orphan outpatient MD administered drugs » HEPZATO is a combination drug device » Kimmtrak (approved for ~45% of mOM population) regulated by CDER – no ANDA pathway priced at an average of $800K per patient and st ended 1 year at >$150M run rate in the US » IP prevents simple 505(B)(2) follow-on » 20 US treatment centers = ~80% patients 6

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![](g422467ex99_1p8g1.jpg)

History of HEPZATO Kit Development 2009 Randomized Phase III Study Completed 2013 FDA Issues a Complete Response Letter 2021 Enrollment for FOCUS Trial Completed Q3/Q4 2023 Commercial Launch HEPZATO Kit 2006 Randomized Phase III Study Begins 2012 Gen 2 Filter CHEMOSAT Granted CE Mark 2016 EU Commercialization Clinical Trial for Patients with Hepatic-Dominant 2023 Ocular Melanoma (FOCUS) PDUFA Date 8/14/23 7

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![](g422467ex99_1p9g1.jpg)

\* First Phase 3 RCT Results - Primary Efficacy Endpoint Met Response Rates Hepatic Progression Free Survival Overall Progression Free Survival (ITT population) (IRC Assessment) (INV Assessment) Proportion of patients surviving Proportion of patients surviving 1.0 3.8 1.0 PHP 5.4 mo PHP PHP BAC P- mo 0.8 Cohort Best alternative care 0.8 Best alternative care (N=44) (N=49) Value 0.6 0.6 hOR 36.4% 2.0% <0.001 5.4 1.6 P<.0001 P<.0001 7.0 0.4 1.6 0.4 ORR 27.3% 4.1% =0.003 0.2 0.2 0.0 0.0 0 5 10 15 20 25 30 35 40 45 50 55 0 5 1 1 2 2 3 0 5 0 5 0 Months Months Hazard Ratio (95% CI) = 0.42 Hazard Ratio (95% CI) = 0.39 Crossover design confounded overall survival analysis – most subjects in BAC arm [57.1%] crossed over to PHP arm \*Mix of mOM and metastatic melanoma with >90% patients diagnosed with mOM - NDA 201848 Clinical Study Report dated 15 August 2012. 8

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![](g422467ex99_1p10g1.jpg)

st Safety Issues from 1 Phase 3 and Resulting Improvements Safety Issues Primarily Due to Filter Improvement Hematological toxicities led to 3 patient deaths Gen 2 Filter introduced in 2013 Gen 1 Gen 2 28 33 % Improvement Adverse Event Adverse Event Hughes 2016 Karydis 2018 Gen 1 → 2 G3/4 G3/4 % n % n Anemia 62.9% 44 Anemia 29.4% 15 53% ¯ Neutropenia 85.7% 60 Neutropenia 31.3% 16 64% ¯ Thrombocytopenia 80.0% 56 Thrombocytopenia 31.3% 16 61% ¯ Inappropriate patient selection and • Protocol amendments were put in place for procedural issues led to 1 patient patient selection death and other AE's • Training improved • ~90% liver involvement causing tumor lysis syndrome FDA required these issues be addressed prior to the start of the FOCUS trial 9

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![](g422467ex99_1p11g1.jpg)

• Multinational, multicenter, single-arm trial • Efficacy Endpoints: FOCUS Trial » Primary: Objective Response Rate (ORR) compared to meta-analysis of IO therapy » Secondary: Duration of Response (DOR), Disease Control Rate (DCR), Overall nd Survival (OS), Progression Free Survival (PFS) 2 Registration Clinical Trial for Patients with • 102 subjects enrolled, 91 completed treatments at 23 centers in the US and EU mOM • HEPZATO Tx every 6-8 weeks up to a maximum of 6 cycles • Initially a RCT against Best Alternative Care (BAC) » Subsequently modified with FDA agreement to single-arm trial 10 » FDA will view the comparisons with the 32 patient BAC arm as supportive exploratory analyses 10

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![](g422467ex99_1p12g1.jpg)

2020 –'23 Initial Approvals Using ORR in Single-Arm Oncology Trials Product Indication N ORR Gavreto (pralsetinib) Metastatic RET NSCLC 114 naïve = 70%, exp. = 57% Monjuvi (tafasitamab-cxix) Relapsed or refractory large B-cell lymphoma 71 39% mutant = 69%, wild-type = Tazverik (tazemetostat) Lymphoma positive for EXH2 mutation 95 34% Zepzelca (lurbinectedin) Metastatic SMLC 2nd Line 105 35% Tabrecta (capmatinib) mNSCLC with mutation MET exon 14 skipping 97 naive = 68%' exp. = 41% Trodelvy (sacituzumab) 3rd Line Metastatic triple-negative BC 108 33.3% Koselugo (selumetinib) Neurofibromatosis Type 1 50 66% Ayvakit (avapritinib) mGIST with PDGFRA exon 18 mutation 43 84% Pemazyre (pemigatinib) Previously treated ICC with FGFR2 fusion 107 36% Fyarro (sirolimus) Malignant perivascular epithelioid cell tumor 31 39% Tivdak (tisotumab vedotin-tftv) 2nd Line cervical cancer 101 24% Exkivity (mobocertinib) mNSCLC w/ EGF mutations 114 28% Jemperli (dostarlimab-gxly) MMRD recurrent or advanced solid tumors – 2nd line 209 41.6% Welireg (belzutifan) von Hippel-Lindau disease +RCC, blastomas, or NET 61 49% Truseltiq (infigratinib) 2nd Line ICC with a FGF 2 fusion 108 23% Lumakras (sotorasib) KRAS G12C mutated mNSCLC 124 36% Rybrevant (amivantamab-vmjw) mNSCLC with EGFR exon 20 insertion mutations 81 40% Jemperli (dostarlimab-gxly) MMRD endometrial cancer, 2nd Line. 71 42.3% Libtayo (cemiplimab-rwlc) Metastatic BCC 112 meta. = 21%, adv. = 29% Tepmetko (tepotinib) mNSCLC w/ met exon 14 152 43% Lunsumio (mosunetuzumab) Relapsed or refractory follicular lymphoma 90 80% Krasati (adagrasib) KRAS G12C-mutated NSCLC 112 38.4% Elahere (mirvetuximab soravtansine-gynx) FRα positive, ovarian, fallopian tube, or primary peritoneal 106 31.7% Jaypirca (pirtobrutinib) Relapsed/refractory mantle cell lymphoma 120 50%

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![](g422467ex99_1p13g1.jpg)

Focus Trial Success Criteria - Informed By FDA Interactions Critical Single Arm Efficacy End Points\* Overall Risk Benefit Assessment • "Clinically Meaningful" ORR\*\* • Significantly improved safety relative to first pivotal trial » Trial powered to show an advantage over immuno- oncology (IO) agents • Positive trends in exploratory BAC comparisons » Lower bound at 95% Confidence Interval needed to (ORR, DOR, DCR, PFS and OS) exceed 8.3% Best Alternative Enrolled Treated • "Clinically Meaningful" DOR\*\*\* Care (BAC) Arm N=42 N=32 » >6 months Dacarbazine 1 0 7 1 Ipilimumab 8 6 Pembrolizumab 26 25 TACE \* Per FDA and SAP ORR is the primary endpoint and per FDA primary analysis population will be treated patient population (SAP defined ITT as primary analysis population) \*\* FDA did not object to using a meta-analysis of checkpoint inhibitors "to provide support for a clinically meaningful ORR" (476 patients from 16 publications, 95% Confidence Interval for ORR of 3.6% - 8.3%) \*\*\* FDA specified that DOR would be the critical secondary endpoint and requested that patients be followed for at least 6 months to assess durability of response 12

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![](g422467ex99_1p14g1.jpg)

FOCUS Trial Analysis: Prespecified Endpoint Met\* ORR Advantage Coupled With Meaningful Duration of Response ORR and DCR in the Treated Population DOR in the Treated Population PHP (n=91) BAC (n=32) † Efficacy Endpoint PHP (n=91) BAC (n=32) p Value Median DOR, months 14 NC ORR, n (%) 33 (36.3) 4 (12.5) [95% CI] [8.31-17.74] [6.93-NC] 0.0133 [95% CI] [26.44, 47.01] [3.51, 28.99] 33 4 Patients with confirmed CR or PR (7 CR, 26 PR) (all PR) DCR, n (%) 67 (73.6) 12 (37.5) Patients with subsequent PD, n (%) 16 (48.5) 1 (25.0) 0.0005 [95% CI] [63.35, 82.31] [21.10, 56.31] Censored, n (%) 17 (51.5) 3 (75.0) † Fisher's Exact Test 26.44% >> 8.3% prespecified threshold\*\* 14 Month Duration of Response Exploratory comparison versus BAC supportive 7 Complete Responses \* 02-Dec-2022 data cut, data continues to mature and patients will be followed at least through May, 2023 \* \* Meta-analysis of checkpoint inhibitors (476 patients,16 publications) calculated a 95% Confidence Interval for ORR of 3.6% - 8.3% 13

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![](g422467ex99_1p15g1.jpg)

Progression Free Survival Kaplan Meier Curves in Treated Populations\* Pre-Specified Exploratory Analyses\* Secondary Endpoint PHP (n=91) BAC (n=32) p Value Median PFS, months 9.03 3.12 † 0.0003 [95% CI] [6.34, 11.56] [2.89, 5.65] PFS status, n (%) Events 67 (73.6) 25 (78.1) Censored 24 (26.4) 7 (21.9) Hazard Ratio Estimate 0.39 ‡ 0.0002 [95% CI] [0.23, 0.63] † Log-Rank test. ‡ Chi-Square test. Exploratory comparison versus BAC supportive \* 02-Dec-2022 data cut, data continues to mature and patients will be followed at least through May, 2023

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![](g422467ex99_1p16g1.jpg)

Overall Survival Kaplan Meier Curves in Treated Populations\* Pre-Specified Exploratory Analyses\* Secondary Endpoint PHP (n=91) BAC (n=32) p Value Median OS, months 20.53 14.49 † 0.1077 [95% CI] [16.79, 25.26] [11.10, 19.78] OS status, n (%) Events 67 (73.6) 25 (78.1) Censored 24 (26.4) 7 (21.9) Hazard Ratio Estimate 0.68 ‡ 0.1110 [95% CI] [0.42, 1.09] † Log-Rank test. ‡ Chi-Square test. Exploratory comparison versus BAC supportive \*\* 02-Dec-2022 data cut, data continues to mature and patients will be followed at least through May, 2023 15

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![](g422467ex99_1p17g1.jpg)

Overall Survival Comparison by Best Overall Response Kaplan Meier Curves in Treated Populations\* Post Hoc Exploratory Analyses\* CR PR SD PD/ND ((N=7) (N=26) N=34) (N=24) Status of OS, N (%) Events 1 (14.3) 17 (65.4) 29 (85.3) 20 (83.3) 6 (85.7) 9 (34.6) 5 (14.7) 4 (16.7) Censored † NC 28.16 19.25 11.99 Median OS (Months) 95% CI [26.71, NC] [23.46, 34.46] [15.90, 23.00] [8.18, 14.03] ‡ p-value <0.0001 CR=complete response, PR=partial response, SD=stable disease, PD=progressive disease, ND=not done, BOR=best overall response Note: NC = Not calculable, due to the number of events within the stratum (n=1) † Kaplan-Meier estimates. ‡ Log-Rank test. \* 02-Dec-2022 data cut, data continues to mature and patients will be followed at least through May, 2023 Analysis Supports that ORR is Clinically Meaningful

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![](g422467ex99_1p18g1.jpg)

Adverse Events Are Predictable and Manageable Related Serious Adverse Events Occurring in >5% of PHP Patients Category, n (%) FOCUS Trial (n=95) Thrombocytopenia\* 14 (14.7%) † Neutropenia 10 (10.5%) Febrile neutropenia 7 (7.4%) ‡ Leukopenia 5 (5.3%) \*Thrombocytopenia includes thrombocytopenia (8, 8.4%) and platelet count decreased (6, 6.3%) † Neutropenia includes neutropenia (8, 8.4%) and neutrophil count decreased (2, 2.1%) ‡ Leukopenia includes leukopenia (4, 4.2%) and white blood cell count decreased (1, 1.1%) 17

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![](g422467ex99_1p19g1.jpg)

Hematological Toxicities - Comparison with Previous Trials\* Grade 3 or higher Adverse Events, FOCUS Trial\* Hughes 2016 Post-procedural (n=91) (n=70) 8 (8.8%) 44 (62.9%) Anemia Thrombocytopenia 27 (29.7%) 56 (80.0%) † Neutropenia 27 (29.7%) 60 (85.7%) Hematological AE's consistent with European experience \*Data cut on 02-Dec-2022 † In the FOCUS Trial, "febrile neutropenia" was included under the category of "neutropenia." In Hughes 2016, "febrile neutropenia" was considered its own category; 12 patients (17.1%) experienced febrile neutropenia. 18

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![](g422467ex99_1p20g1.jpg)

FOCUS Trial – Safety Comparison with Previous Trials\* FOCUS Trial Pooled Analysis of Category (N=95) Prior Studies (N=121) Patients who Withdrew due to an AE or 17 (17.9%) 46 (38%) SAE Patients who Received a Reduced Dose 12 (12.6%) 27 (22.3%) due to an AE or SAE 4.1 2.8 Average Number of Cycles Improvement in tolerability led to a larger number of treatments \* Data cut on 02-Dec-2022 19

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![](g422467ex99_1p21g1.jpg)

FOCUS Trial Comparison to Other Published Studies\* Median OS Median PFS Clinical Study Type Treatment (months) (months) N Study/Publication (95% CI) (95% CI) AL 91 20.53 9.03 FOCUS Single-Arm Hepzato (16.79 to 25.26) (6.34 to 11.56) 13 Khoja et al 2019 systemic and liver-directed 10.2 3.3 Meta-Analysis 912 (based on 29 therapies (9.5 to 11.0) (2.9 to 3.6) articles) 14 Rantala et al 2019 systemic and liver-directed 12.84 Meta-Analysis 2494 - (based on 78 therapies (12.00 to 13.56) articles) 12.7 3.0 11 TN Piulats et al 2021 Single-Arm ipilimumab plus nivolumab 52 (7.1 to 18.3) (2 to 4.1) ipilimumab + (pembrolizumab AL Heppt et al 2019 Single-Arm 64 16.1 3.0 or nivolumab) 21.7 3.3 TN tebentafusp 252 (18.6 to 28.6) (3 to 5) 9 Nathan et al 2021 Randomized 16 2.9 TN control 126 (9.7 to 18.4) (2.8 to 3) TN = Treatment Naïve, AL = Any Line \*Studies from 2019 or later with >50 patients

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![](g422467ex99_1p22g1.jpg)

Expanded Access Program (EAP) Institution City Principal Investigator Status Moffitt Cancer Center Tampa, Florida Dr. Jonathan Zager Open and Enrolling Duke University Durham, North Carolina Dr. Georgia Beasley Open and Enrolling University of Tennessee Memphis, Tennessee Dr. Evan Glazer Open and Enrolling Contract and budget are under review Thomas Jefferson University Philadelphia, Pennsylvania Dr. Marlana Orloff with the site Contract and budget are under review Stanford University Stanford, California Dr. Sunil Reddy with the site Contract and budget are under review Ohio State University Columbus, Ohio Dr. Aslam Ejaz with the site Mayo Clinic Hospital Jacksonville, Florida Dr. Roxana Dronca / Dr. Yiyi Yan Contract and budget discussions initiated Interested to participate in EAP; need Emory University Atlanta, Georgia Dr. Mike Lowe additional time to start activities Interested to participate in EAP; need University of Miami Miami, Florida Dr. Jose Lutzky additional research staff before participating 21

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![](g422467ex99_1p23g1.jpg)

mOM Beachhead Market Strategy BEACHHEAD MARKET \| mOM LIVER DISEASE SIGNIFICANT REVENUE OPPORTUNITY: • Oncologists\* believe ~80% of mOM patients would be HEPZATO candidates - ~800 patients US TAM • Considered a significant advancement >$450M • Payer & hospital finance stakeholders suggest pricing expectations in the per year range of IO agents • Tebentafusp is priced at an estimated ~$820 per patient\*\* and generated rd $50M in global revenue in the 3 full quarter post launch • May be positioned as a first-line treatment due to limited efficacy of available therapies. \*Source: Boston Health Associates primary research n=13 physicians, \*\* $400K consensus estimates from Immunocore's covering analysts assuming treatment until progression, $1M annualized cost assuming treatment through progression (25% longer duration than pivotal trial) 22

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![](g422467ex99_1p24g1.jpg)

Specialized, Targeted Sales Team Leveraging EAP and Longitudinal Data EAP (FDA Approved) – Up to 8 Sites • Provide immediate access to patients • First Commercial Sites • Train new medical teams to use Hepzato after launch Regional Based Sales Team • Experienced, Oncology focused • Upon launch, placed in key geographies • Supplement with Clinical Support Specialist Leverage Longitudinal Data • Partnered with data provider to access patient level longitudinal data with 3-week refresh Planned EAP sites • Accurately map and quantify surveillance, referral and treatment patterns at the patient and MD level Potential Hepzato Treatment Sites 23

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![](g422467ex99_1p25g1.jpg)

Reimbursement HEPZATO will be billed as a drug with a J-Code • Medicare Patients • Initially a C-Code • Majority of patients will be outpatient (2 midnight rule) with the drug directly covered by Medicare • Private Payer Patients • Private Payers for rare disease generally follow Medicare guidelines and we expect these patients to be treated as outpatients • Prior-Authorization of patients might be needed, we are planning to contract out a hub service • Centers of Excellence (PPS exempt and NCI designated Cancer Centers) have the leverage to negotiate favorable rates and reimbursement terms (our target sites are all either PPS exempt or NCI Cancer Centers) 24

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PHP Is ALREADY Part of Current NCCN Guidelines for mOM Regional Isolation Perfusion Methods include isolated hepatic infusion (IHP), percutaneous hepatic perfusion (PHP), HAI, and embolization techniques. PHP is a simpler, less invasive alternative to IHP that can be repeated. It uses a double-balloon catheter inserted into the inferior vena cava to isolate hepatic venous blood that is then filtered extracorporeally. 25

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Components of Hospital Reimbursement Assuming Outpatient Pass Through Status with C Code CPT Code mapping underway – while Drug Healthcare Facility "Physician" payment important, it will not Fee have a meaningful • ASP+6% (CMS) • Actually goes to hospital impact on drug but still matters to MD • Highly variable based • Likely similar for pricing decision on coding – we do not commercial payers • Highly variable based "map" to any existing on coding – we do not code "map" to any existing code • Using existing codes is advised and should • Using existing codes is provide the hospital advised and should adequate payment provide the hospital adequate payment 26

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Hepzato vs. Kimmtrak Cost of Treatment Comparisons At First Assessment (first time to discontinue treatment because of progression) Drug Dose Cost Treatments # Total cost Kimmtrak $20,261 24 $486,264 Hepzato t.b.d. 2 t.b.d. Mean Hepzato treatment vs. mean treatment duration of Kimmtrak Drug Dose Cost Mean Treatments # Total cost Kimmtrak $20,261 41 $830,701 Hepzato t.b.d. 4.1 t.b.d. 27

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Rapid Uptake for FDA Approved Treatment in mOM • Demonstrated demand for FDA approved treatments for mOM Kimmtrak US Quarterly Sales – Kimmtrak - $38 million in Q4 2022 US sales ($152M annualized revenue) (USD) – Only 45% of mOM patients are eligible for treatment with Kimmtrak (unique MOA) $40,000,000 – Kimmtrak has an estimated 40% share of eligible patients in less than 12 months $30,000,000 $20,000,000 $10,000,000 • Hepzato Kit submitted for FDA approval 14 February 2023 $0 – 100% of mOM patients are eligible for treatment with Hepzato Q1 2022 Q2 2022 Q3 2022 Q4 2022 – Hepzato will require <20% of eligible patients to achieve similar 4 quarter growth\* US Quarterly Sales USD • Hepzato Kit is well positioned to generate rapid uptake % of TAM to Achieve Similar – Hepzato is more of a complement than a competitor to Kimmtrak for patients eligible for Kimmtrak Revenue Growth – Hepzato can treat all mOM patients and will be the only FDA approved drug for 55% of 60 patients st st 40 – Hepzato EAP patients have included: 1 line stand alone treatment, 1 line treatment for nd rd those intending to receive Kimmtrak, as 2 line treatment, and as a 3 line palliative 20 treatment 0 – NCCN Guidelines currently state "regional isolation perfusion of the liver" as a Q1 2022 Q2 2022 Q3 2022 Q4 2022 recommended treatment Kimmtrack Hepzato – "If disease is confined to the liver, regional therapies…should be considered. Since tebentafusp-tebn response rates are low, symptomatic patients may be better palliated by liver-directed treatment first…." NCCN Guidelines Melanoma Uveal V2.2022 \* Assuming $150K per treatment and 4 treatments per patient. 28

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IO Combination Proof of Principal – Ongoing CHOPIN Trial • N=7 in Phase 1b portion of the trial (mOM patients) • 1CR, 6 PR and 1 PD (85.7% ORR, 100% DCR) – meta-analysis of prior IO trials has shown ORR<<10% • As of 11/15/22 the median follow-up was 29.1 months (range 8.9 – 30.2), the median PFS was 29.1 months (95% CI 11.9 – 46.3) and the median duration of response was 27.1 months (range 7.4 – 28.5) • All patients are still alive 29 • 3 of 4 patients who subsequently experienced PD continued with treatment in the form of repeated Melphalan Chemosat treatments • The safe treatment dose was established at IPI 1mg/kg and NIVO 3mg/kg. • Both cohorts were tolerated with no dose-limiting toxicities or deaths • Ongoing randomized Phase 2 (control is Chemosat) has recruited 50% of N=76 patients and will provide an interim analysis at N=40 patients Published 09 January 2023 in Cardiovascular and Interventional Radiology: https://doi.org/10.1007/s00270-022-03338-1 29

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The Local Hepatic Myeloablative Effect May Improve IO Efficacy 30

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EU – Broad Reimbursement Pending Focus Trial Data; Demonstrated Interest Across Multiple Indications » CE Marked - available in ~23 centers in 4 countries » Delcath resumed direct sales on 3/1/22 CHEMOSAT Used In 13 Tumor Types ~70%: Metastatic Ocular Melanoma (mOM) » NICE (UK) upgraded status from "Research" to "Special Status" Other Types Treated: » German reimbursement based on annual • Intrahepatic Cholangiocarcinoma (ICC) hospital special request ("ZE" process) • Hepatocellular Carcinoma (HCC) • Metastatic Colorectal Cancer (mCRC) • Metastatic Breast (mBreast) » Strong interest to fuel additional indications • Pancreatic driven by HCP's • Metastatic Neuroendocrine Tumors (mNET) • Metastatic Cutaneous Melanoma (mCM) » 1,343 commercial Chemosat kits shipped to the EU » Queensbury facility has been inspected 21 times by the Notified Bodies LRQA and BSI, Health Authorities FDA and ANVISA 31

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IHP Results in mOM Provided Rationale for PHP in mOM and Provides Rationale for CRC and Other Tumor Types 18-22 IHP/mOM ORR 23-29 IHP/CRC ORR 80% 80% 70% 68% 70% 61% 60% 62% 62% 59% 60% 60% 50% 50% 47% 50% 41% 40% 40% 29% 30% 20% 20% 10% 0% 0% n=105 n=71 n=29 n=99 n=120 n=24 n=30\* n=34 n=17 n=27 n=22 n=25\* Category 1 Category 1 IHP Studies in other disease states • Primary HCC and ICC utilizing IHP (melphalan +/- TNF alpha). ORR = 67% (N=13) with a median 30 actuarial survival of 16.3 months. • Unresectable GEP-NET utilizing IHP (melphalan +/- TNF alpha). ORR = 50% (N=13) with a median 31 actuarial survival of 48 months. \*Hepatic arterial infusion used adjunctively. 32 ORR % ORR %

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Clinical Rationale for Broad Development Effort "Broad-spectrum" alkylating • Promising ORR and DCR signals seen across agent given at 12X normal multiple tumor types in Europe and in earlier systemic doses studies with IHP • When the liver is the life limiting organ, systemic chemotherapy can be paused and HEPZATO Liver mets are often life added to prolong survival limiting and reduce I/O efficacy • Early data supports that combination with I/O agents is safe and effective • For patients at high risk of liver mets based on PHP treats the entire liver and tumor characteristics or ctDNA, adjuvant is not dependent on tumor therapy is logical location 33

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Market Expansion: Significant Investigator Interest Possible Areas for Further Hepzato Development\* Combination Therapy – IO Agents Limited, but 50,000 High Unmet Need IHP Efficacy Well 28 Documented 40,000 Limited, but US TAM High Unmet Need 30,000 ~10 EU 27 >$1B Cases 20,000 Phase 2 Data Per Year Extensive EU 26 Experience 10,000 FOCUS Trial 0 mOM ICC mBC mNET mPC mCRC HCC Liver Dominant Cancers 1,2 3,4 7-10 \*Metastatic Ocular Melanoma (mOM) , Cholangiocarcinoma (ICC) , Liver-dominant Breast Cancer (mBC) , Metastatic Neuroendocrine 34 6,7 7,13 11,12 15 Tumors (mNET) Metastatic Pancreatic Cancer (mPC) , Metastatic Colorectal Cancer (mCRC) , Hepatocellular carcinoma (HCC) U.S. Incidence

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Multi-Disciplinary, Experienced Leadership Team GERARD MICHEL JOHN PURPURA Chief Executive Officer Chief Operating Officer » Past VP and Exec Director roles of Reg. » 30+ yrs. pharma/medtech experience Affairs for Bracco Diagnostics » C-suite roles at Vericel Corp, Biodel, & NPS » Held senior roles Sanofi-Aventis, Bolar » M.S. Microbiology, B.S. Biology & Geology Pharma, Luitpold Pharma & Eon Labs from the Univ. of Rochester School of BOARD OF DIRECTORS » M.S. Mgmnt. & Policy and B.S. Medicine Chemistry and Biology at the State » M.B.A. Simon School of Business & John R. Sylvester Chairman University of NY at Stony Brook Leadership Dr. Roger G. Stoll, Ph.D. Director Elizabeth Czerepak Director Steven Salamon Director KEVIN MUIR JOHNNY JOHN, MD Dr. Gil Aharon, Ph.D. Director VP, Commercial Operations SVP Clinical Development & Medical Affairs Gerard Michel CEO » 20+ yrs. of medtech/bioTx sales & » 15+ yrs. experience in oncology drug marketing experience. development and clinical trials » Held senior leadership roles at BTG, » 11 years of personal clinical practice ClearFlow, Aragon Surgical, Kensey Nash » Received M.D. from Mangalore Corporation, and Kyphon. University, India; post-grad training at » Field Artillery officer in the U.S. Army the University of IL » B.S. in Management Systems Engineering at the U.S. Military Academy at West Point 35

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Capital Structure and Share Information Material One Time Q1 Events 12/31/22 1, 2 Incremental (+/-) Changes 3 1 12.72 +7.58 Shares Outstanding 1 +$23.5M Cash and Cash $11.8M 2 Equivalents -$4M 4 1 3.61M +11.94M Warrants Outstanding 2.34M NA Stock Options Granted $25.0M NA 2022 Cash Burn 5 1 $16.9M -$4M Debt 6 $2.59 - $7.95 NA 52 week Low – High 30d Average Daily 7 22,960 NA Volume 1 Includes a $4M prepayment of debt 2 Includes $25M PIPE financing for 7.58 Series F Pfd shares, 7.78M Tranche A warrants for an aggregate exercise price $34.9 million exercisable until the earlier of 3/31/2026 or 21 days receipt of FDA approval for HEPZATO; and 4.17M Tranche B warrants for an aggregate exercise price $24.9 million exercisable until the earlier of 3/31/2026 or 21 days following recording at least $10 million in quarterly U.S. revenue. 3 As of December 31, 2022; includes 10.0M of Common plus 1.1M, Preferred E & E-1 & 1.5M Pre-funded Warrants as converted 4 $10 exercise price 5 Includes $5.0M of notes convertible at $11.98 per common share equivalent 6 Used NASDAQ price information starting on January 1, 2022- December 31, 2022 7 30-day average calculated between November 17, 2022 - December 30, 2022 36

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Delcath: Investment Summary 3Q approval in mOM likely due to strong pivotal data and real-world experience Kimmtrak proving out significant commercial opportunity ($200M run rate) with 45% of the HEPZATO TAM Rapid uptake likely due to favorable reimbursement environment, NCCN guidelines including PHP and equivalent OS as Kimmtrack in more advance patient population Management team experienced in commercializing high value, specialty products Multiple 2023 catalysts (AdCom, Approval, CHOPIN data) High value follow-on indications and strategic interest creates significant upside 37

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THANK YOU 38 38

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References 1. Cancer.net Editorial Board (2020) Eye Cancer - Statistics. In: Cancer.Net. https://www.cancer.net/cancer-types/eye-cancer/statistics. Accessed 22 Jun 2020. 2. Ocular Melanoma Foundation. Treatment of Metastatic Disease. In: OMF – Metastatic Treatment. http://www.ocularmelanoma.org/metstreatment.htm. Accessed 22 Jun 2020. 3. Patel N, Benipal B. Incidence of Cholangiocarcinoma in the USA from 2001 to 2015: A US Cancer Statistics Analysis of 50 States. Cureus. 2019;11(1):e3962. Published 2019 Jan 25. 4. United States Census Bureau. (2019) Monthly Population Estimates for the United States: April 1, 2010 to December 1, 2020 (NA-EST2019-01). 5. Cancer.net Editorial Board. (2020) Neuroendocrine Tumors - Statistics. In: Cancer.Net. https://www.cancer.net/cancer-types/neuroendocrine-tumors/statistics. Accessed 22 Jun 2020. 6. Saeed A, Buell JF, Kandil E. Surgical treatment of liver metastases in patients with neuroendocrine tumors. Ann Transl Med. 2013;1(1):6. doi:10.3978/j.issn.2305- 5839.2013.01.08. 7. Surveillance, Epidemiology, and End Results (SEER) Program Populations (1969-2018) (www.seer.cancer.gov/popdata), National Cancer Institute, DCCPS, Surveillance Research Program, released December 2019. 8. Adam R, Aloia T, Krissat J, Bralet MP, Paule B, Giacchetti S, Delvart V, Azoulay D, Bismuth H, Castaing D. Is liver resection justified for patients with hepatic metastases from breast cancer? Ann Surg. 2006 Dec;244(6):897-907; discussion 907-8. doi: 10.1097/01.sla.0000246847.02058.1b. PMID: 17122615; PMCID: PMC1856635. 9. Insa A, Lluch A, Prosper F, Marugan I, Martinez-Agullo A, Garcia-Conde J. Prognostic factors predicting survival from first recurrence in patients with metastatic breast cancer: analysis of 439 patients. Breast Cancer Res Treat. 1999 Jul;56(1):67-78. doi: 10.1023/a:1006285726561. PMID: 10517344. 10. Clark GM, Sledge GW Jr, Osborne CK, McGuire WL. Survival from first recurrence: relative importance of prognostic factors in 1,015 breast cancer patients. J Clin Oncol. 1987 Jan;5(1):55-61. doi: 10.1200/JCO.1987.5.1.55. PMID: 3806159. 11. Cancer.net Editorial Board. (2020) Colorectal Cancer - Statistics. In: Cancer.Net. https://www.cancer.net/cancer-types/colorectal-cancer/statistics. Accessed 22 Jun 2020. 12. Ismaili N. Treatment of colorectal liver metastases. World J Surg Oncol. 2011;9:154. Published 2011 Nov 24. doi:10.1186/1477-7819-9-154. 13. Oweira H, Petrausch U, Helbling D, Schmidt J, Mannhart M, Mehrabi A, Schöb O, Giryes A, Decker M, Abdel-Rahman O. Prognostic value of site-specific metastases in pancreatic adenocarcinoma: A Surveillance Epidemiology and End Results database analysis. World J Gastroenterol. 2017 Mar 14;23(10):1872-1880. doi: 10.3748/wjg.v23.i10.1872. PMID: 28348494; PMCID: PMC5352929. 39

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References 14. Key Statistics About Liver Cancer. American Cancer Society. Facts & Figures 2021. American Cancer Society. Atlanta, Ga. 2021. Key Statistics About Liver Cancer. American Cancer Society. Facts and Figures 2021. American Cancer Society. Atlanta, GA 2021. 15. Isolated hepatic perfusion for patients with liver metastases, Ther Adv Med Oncol. 2014 Jul; 6(4): 180-194. 16. Tulokas S, Mäenpää H, et al. Selective internal radiation therapy (SIRT) as treatment for hepatic metastases of uveal melanoma: a Finnish nation-wide retrospective 17. Shibayama Y, Namikawa K, Sone M, et al. Efficacy and toxicity of transarterial chemoembolization therapy using cisplatin and gelatin sponge in patients with liver metastases from uveal melanoma in an Asian population. Int J Clin Oncol. 2017 Jun;22(3):577-584. doi: 10.1007/s10147-017-1095-0. Epub 2017 Jan 31. PMID: 28144882 18. Olofsson R, Ny L, Eilard MS, et al. Isolated hepatic perfusion as a treatment for uveal melanoma liver metastases (the SCANDIUM trial): study protocol for a randomized controlled trial. Trials. 2014; 15:317. 19. Varghese S, Xu H, Bartlett D, et al. Isolated hepatic perfusion with high-dose melphalan results in immediate alterations in tumor gene expression in patients with metastatic ocular melanoma. Ann Surg Oncol. 2010;17:1870–7. 20. Rizell M, Mattson J, Cahlin C, Hafstrom L, Lindner P, Olausson M. Isolated hepatic perfusion for liver metastases of malignant melanoma. Melanoma Res. 2008;18:120–6. 21. Alexander HR, Libutti SK, Bartlett DL, Puhlmann M, Fraker DL, Bachenheimer LC. A phase I-II study of isolated hepatic perfusion using melphalan with or without tumor necrosis factor for patients with ocular melanoma metastatic to liver. Clin Cancer Res. 2000;6:3062–70. 22. Alexander HR, Libutti SK, Pingpank JF, Steinberg SM, Bartlett DL, Helsabeck C, Beresneva T. Hyperthermic isolated hepatic perfusion using melphalan for patients with ocular melanoma metastatic to the liver. Clinical Cancer Res. 2003;9, 6343-49. 23. van Iersel LB, Koopman M, van de Velde CJ, et al. Management of isolated nonresectable liver metastases in colorectal cancer patients: a case-control study of isolated hepatic perfusion with melphalan versus systemic chemotherapy. Ann Oncol. 2010;21:1662–7. 24. Alexander HR Jr, Bartlett DL, Libutti SK, et al. Analysis of factors associated with outcome in patients undergoing isolated hepatic perfusion for unresectable liver metastases from colorectal center. Ann Surg Oncol. 2009;16:1852–9. 25. van Iersel LB, Gelderblom H, Vahrmeijer AL, et al. Isolated hepatic melphalan perfusion of colorectal liver metastases: outcome and prognostic factors in 154 patients. Ann Oncol. 2008;19:1127–34. 26. Rothbarth J, Pijl ME, Vahrmeijer AL, et al. Isolated hepatic perfusion with high-dose melphalan for the treatment of colorectal metastasis confined to the liver. Br J Surg. 2003;90:1391–7. 40

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References 27. Vahrmeijer AL, van Dierendonck JH, Keizer HJ, et al. Increased local cytostatic drug exposure by isolated hepatic perfusion: a phase I clinical and pharmacologic evaluation of treatment with high dose melphalan in patients with colorectal cancer confined to the liver. Br J Cancer. 2000;82:1539–46. 28. Alexander HR Jr, Libutti SK, Pingpank JF, Bartlett DL, Helsabeck C, Beresneva T. Isolated hepatic perfusion for the treatment of patients with colorectal cancer liver metastases after irinotecan-based therapy. Ann Surg Oncol. 2005;12:138–44. 29. Van Iersel LB, Verlaan MR, Vahrmeijer AL, et al. Hepatic artery infusion of high-dose melphalan at reduced flow during isolated hepatic perfusion for the treatment of colorectal metastases confined to the liver: a clinical and pharmacologic evaluation. Eur J Surg Oncol. 2007;33:874–81. 30. Hughes S., et al. Ann Surg Oncol. 2016 Apr;23(4):1309-19. doi: 10.1245/s10434-015-4968-3.8-3. 31. Sacco J, et al. Annals of Oncology (Dec 2020) 31 (suppl_7): S1441-S1451. 10.1016/annonc/annonc392 32. Bethlehem M., et al. Meta-analysis of Isolated Hepatic Perfusion and Percutaneous Hepatic Perfusion as a Treatment for Uveal Melanoma Liver Metastases. Cancers 2021, 13(18), 4726; 33. de Leede E., et al. Cardiovascular Intervent Radiol. 2017 Aug;40(8):1196-1205. 34. Xu L, T, Funchain P, F, Bena J, F, Li M, Tarhini A, Berber E, Singh A, D: Uveal Melanoma Metastatic to the Liver: Treatment Trends and Outcomes. Ocul Oncol Pathol 2019;5:323-332. doi: 10.1159/000495113. 35. Lane AM, Kim IK, Gragoudas ES. Survival Rates in Patients After Treatment for Metastasis From Uveal Melanoma. JAMA Ophthalmol. 2018 Sep 1;136(9):981- 986. 36. Karydis I, Gangi A, Wheater MJ, et al. Percutaneous hepatic perfusion with Melphalan in uveal melanoma: A safe and effective treatment modality in an orphan disease. J Surg Oncol. 2018;117(6):1170-1178. doi:10.1002/jso.24956 37. FOCUS trial data 12/14/22. 38. Meta-analysis: Data on file 41