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Complementary dual-virus strategy drives synthetic target and cognate T-cell engager expression for endogenous-antigen agnostic immunotherapy.


ABSTRACT: Targeted antineoplastic immunotherapies have achieved remarkable clinical outcomes. However, resistance to these therapies due to target absence or antigen shedding limits their efficacy and excludes tumours from candidacy. To address this limitation, here we engineer an oncolytic rhabdovirus, vesicular stomatitis virus (VSVΔ51), to express a truncated targeted antigen, which allows for HER2-targeting with trastuzumab. The truncated HER2 (HER2T) lacks signaling capabilities and is efficiently expressed on infected cell surfaces. VSVΔ51-mediated HER2T expression simulates HER2-positive status in tumours, enabling effective treatment with the antibody-drug conjugate trastuzumab emtansine in vitro, ex vivo, and in vivo. Additionally, we combine VSVΔ51-HER2T with an oncolytic vaccinia virus expressing a HER2-targeted T-cell engager. This dual-virus therapeutic strategy demonstrates potent curative efficacy in vivo in female mice using CD3+ infiltrate for anti-tumour immunity. Our findings showcase the ability to tailor the tumour microenvironment using oncolytic viruses, thereby enhancing compatibility with "off-the-shelf" targeted therapies.

SUBMITTER: Taha Z 

PROVIDER: S-EPMC11343834 | biostudies-literature | 2024 Aug

REPOSITORIES: biostudies-literature

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Complementary dual-virus strategy drives synthetic target and cognate T-cell engager expression for endogenous-antigen agnostic immunotherapy.

Taha Zaid Z   Crupi Mathieu Joseph François MJF   Alluqmani Nouf N   MacKenzie Duncan D   Vallati Sydney S   Whelan Jack Timothy JT   Fareez Faiha F   Alwithenani Akram A   Petryk Julia J   Chen Andrew A   Spinelli Marcus Mathew MM   Ng Kristy K   Sobh Judy J   de Souza Christiano Tanese CT   Bharadwa Priya Rose PR   Lee Timothy Kit Hin TKH   Thomas Dylan Anthony DA   Huang Ben Zhen BZ   Kassas Omar O   Poutou Joanna J   Gilchrist Victoria Heather VH   Boulton Stephen S   Thomson Max M   Marius Ricardo R   Hooshyar Mohsen M   McComb Scott S   Arulanandam Rozanne R   Ilkow Carolina Solange CS   Bell John Cameron JC   Diallo Jean-Simon JS  

Nature communications 20240823 1


Targeted antineoplastic immunotherapies have achieved remarkable clinical outcomes. However, resistance to these therapies due to target absence or antigen shedding limits their efficacy and excludes tumours from candidacy. To address this limitation, here we engineer an oncolytic rhabdovirus, vesicular stomatitis virus (VSVΔ51), to express a truncated targeted antigen, which allows for HER2-targeting with trastuzumab. The truncated HER2 (HER2T) lacks signaling capabilities and is efficiently ex  ...[more]

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