Litcius/Paper detail

Phase I study of VSV-GP (BI 1831169) as monotherapy or combined with ezabenlimab in advanced and refractory solid tumors

Mercedes Porosnicu, Anne‐Marie Quinson, Kate Crossley, Stephan Luecke, Ulrich M. Lauer

2022Future Oncology31 citationsDOIOpen Access PDF

Abstract

Patients with advanced, recurrent or metastatic cancer have poor prognosis despite treatment advancements. Vesicular stomatitis virus (VSV)-glycoprotein (GP; BI 1831169) is a chimeric VSV with its neurotropic glycoprotein G replaced by the non-neurotropic GP of the lymphocytic choriomeningitis virus. This live, recombinant oncolytic virus has demonstrated preclinical efficacy as a viral-based immunotherapy due to its interferon-dependent tumor specificity, potent oncolysis and stimulation of antitumor immune activity. Co-administration of the immune checkpoint inhibitor, ezabenlimab (BI 754091), alongside VSV-GP may synergistically enhance antitumor immune activity. Here, we describe the rationale and design of the first-in-human, phase I, dose-escalation study of VSV-GP alone and in combination with the immune checkpoint inhibitor ezabenlimab in patients with advanced, metastatic or relapsed and refractory solid tumors (NCT05155332).

Topics & Concepts

Oncolytic virusVesicular stomatitis virusImmune systemMedicineImmunotherapyImmune checkpointVirotherapyVirologyCancerImmunologyVirusLymphocytic choriomeningitisCancer researchInternal medicineCD8Virus-based gene therapy researchCAR-T cell therapy researchViral Infections and Outbreaks Research