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Cancer Immunology Research
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Research Article

ONCR-177, an Oncolytic HSV-1 Designed to Potently Activate Systemic Antitumor Immunity

Brian B Haines, Agnieszka Denslow, Peter Grzesik, Jennifer S Lee, Terry Farkaly, Jacqueline Hewett, Daniel Wambua, Lingxin Kong, Prajna Behera, Judith Jacques, Caitlin Goshert, Michael Ball, Allison Colthart, Mitchel H. Finer, Melissa W Hayes, Sonia Feau, Edward M. Kennedy, Lorena Lerner and Christophe Quéva
Brian B Haines
1Pharmacology-Toxicology, ONCORUS
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  • For correspondence: brian.haines@oncorus.com
Agnieszka Denslow
2Oncorus
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Peter Grzesik
2Oncorus
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Jennifer S Lee
3Molecular Biology and Virology, Oncorus
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  • ORCID record for Jennifer S Lee
Terry Farkaly
2Oncorus
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Jacqueline Hewett
2Oncorus
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Daniel Wambua
2Oncorus
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Lingxin Kong
2Oncorus
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Prajna Behera
4Neuroscience and Physiology, SUNY Upstate Medical University
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Judith Jacques
2Oncorus
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Caitlin Goshert
2Oncorus
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Michael Ball
2Oncorus
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Allison Colthart
2Oncorus
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Mitchel H. Finer
5Basecamp, Elevate Bio
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Melissa W Hayes
6Immunology, Oncorus
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Sonia Feau
2Oncorus
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Edward M. Kennedy
2Oncorus
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Lorena Lerner
7Molecular Biology & Virology, Oncorus
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Christophe Quéva
2Oncorus
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DOI: 10.1158/2326-6066.CIR-20-0609
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Abstract

ONCR-177 is an engineered recombinant oncolytic herpes simplex virus (oHSV) with complementary safety mechanisms, including tissue-specific microRNA (miR) attenuation and mutant UL37 to inhibit replication, neuropathic activity, and latency in normal cells. ONCR-177 is armed with five transgenes for IL12, FLT3LG (extracellular domain [ECD]), CCL4, and antagonists to immune checkpoints PD-1 and CTLA-4. In vitro assays demonstrated that targeted miRs could efficiently suppress ONCR-177 replication and transgene expression, as could the HSV-1 standard-of-care therapy acyclovir. Although ONCR-177 was oncolytic across a panel of human cancer cell lines, including in the presence of type I interferon, replication was suppressed in human pluripotent stem cell (iPSC)-derived neurons, cardiomyocytes, and hepatocytes. Dendritic cells activated with ONCR-177 tumor lysates efficiently stimulated tumor antigen-specific CD8+ T-cell responses. In vivo, biodistribution analyses suggested that viral copy number and transgene expression peaked approximately 24-72 hours post injection and remained primarily within the injected tumor. Intratumoral (IT) administration of ONCR-177 mouse surrogate virus, mONCR-171, was efficacious across a panel of syngeneic bilateral mouse tumor models, resulting in partial or complete tumor regressions that translated into significant survival benefits and to the elicitation of a protective memory response. Antitumor effects correlated with local and distant IT infiltration of several immune effector cell types, consistent with the proposed functions of the transgenes. The addition of systemic anti-PD-1 augmented the efficacy of mONCR-171, particularly for abscopal tumors. Based in part upon these preclinical results, ONCR-177 is being evaluated in patients with metastatic cancer (ONCR-177-101, NCT04348916).

  • Received July 16, 2020.
  • Revision received September 25, 2020.
  • Accepted December 18, 2020.
  • Copyright ©2020, American Association for Cancer Research.

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This OnlineFirst version was published on December 22, 2020
doi: 10.1158/2326-6066.CIR-20-0609

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ONCR-177, an Oncolytic HSV-1 Designed to Potently Activate Systemic Antitumor Immunity
Brian B Haines, Agnieszka Denslow, Peter Grzesik, Jennifer S Lee, Terry Farkaly, Jacqueline Hewett, Daniel Wambua, Lingxin Kong, Prajna Behera, Judith Jacques, Caitlin Goshert, Michael Ball, Allison Colthart, Mitchel H. Finer, Melissa W Hayes, Sonia Feau, Edward M. Kennedy, Lorena Lerner and Christophe Quéva
Cancer Immunol Res December 22 2020 DOI: 10.1158/2326-6066.CIR-20-0609

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ONCR-177, an Oncolytic HSV-1 Designed to Potently Activate Systemic Antitumor Immunity
Brian B Haines, Agnieszka Denslow, Peter Grzesik, Jennifer S Lee, Terry Farkaly, Jacqueline Hewett, Daniel Wambua, Lingxin Kong, Prajna Behera, Judith Jacques, Caitlin Goshert, Michael Ball, Allison Colthart, Mitchel H. Finer, Melissa W Hayes, Sonia Feau, Edward M. Kennedy, Lorena Lerner and Christophe Quéva
Cancer Immunol Res December 22 2020 DOI: 10.1158/2326-6066.CIR-20-0609
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