Frontiers in Immunology (Oct 2023)

A phase I oncolytic virus trial with vesicular stomatitis virus expressing human interferon beta and tyrosinase related protein 1 administered intratumorally and intravenously in uveal melanoma: safety, efficacy, and T cell responses

  • Katherine E. R. Smith,
  • Kah-Whye Peng,
  • Jose S. Pulido,
  • Adam J. Weisbrod,
  • Carrie A. Strand,
  • Jacob B. Allred,
  • Alysha N. Newsom,
  • Lianwen Zhang,
  • Nandakumar Packiriswamy,
  • Timothy Kottke,
  • Jason M. Tonne,
  • Madelyn Moore,
  • Heather N. Montane,
  • Lisa A. Kottschade,
  • Robert R. McWilliams,
  • Arkadiusz Z. Dudek,
  • Yiyi Yan,
  • Anastasios Dimou,
  • Svetomir N. Markovic,
  • Mark J. Federspiel,
  • Richard G. Vile,
  • Roxana S. Dronca,
  • Matthew S. Block

DOI
https://doi.org/10.3389/fimmu.2023.1279387
Journal volume & issue
Vol. 14

Abstract

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IntroductionMetastatic uveal melanoma (MUM) has a poor prognosis and treatment options are limited. These patients do not typically experience durable responses to immune checkpoint inhibitors (ICIs). Oncolytic viruses (OV) represent a novel approach to immunotherapy for patients with MUM.MethodsWe developed an OV with a Vesicular Stomatitis Virus (VSV) vector modified to express interferon-beta (IFN-β) and Tyrosinase Related Protein 1 (TYRP1) (VSV-IFNβ-TYRP1), and conducted a Phase 1 clinical trial with a 3 + 3 design in patients with MUM. VSV-IFNβ-TYRP1 was injected into a liver metastasis, then administered on the same day as a single intravenous (IV) infusion. The primary objective was safety. Efficacy was a secondary objective.Results12 patients with previously treated MUM were enrolled. Median follow up was 19.1 months. 4 dose levels (DLs) were evaluated. One patient at DL4 experienced dose limiting toxicities (DLTs), including decreased platelet count (grade 3), increased aspartate aminotransferase (AST), and cytokine release syndrome (CRS). 4 patients had stable disease (SD) and 8 patients had progressive disease (PD). Interferon gamma (IFNγ) ELIspot data showed that more patients developed a T cell response to virus encoded TYRP1 at higher DLs, and a subset of patients also had a response to other melanoma antigens, including gp100, suggesting epitope spreading. 3 of the patients who responded to additional melanoma antigens were next treated with ICIs, and 2 of these patients experienced durable responses.DiscussionOur study found that VSV-IFNβ -TYRP1 can be safely administered via intratumoral (IT) and IV routes in a previously treated population of patients with MUM. Although there were no clear objective radiographic responses to VSV-IFNβ-TYRP1, dose-dependent immunogenicity to TYRP1 and other melanoma antigens was seen.

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