Alternating Arenavirus Vector Immunization Generates Robust Polyfunctional Genotype Cross-Reactive Hepatitis B Virus–Specific CD8 T-Cell Responses and High Anti–Hepatitis B Surface Antigen Titers

Author:

Schmidt Sarah1,Mengistu Meron2,Daffis Stephane2,Ahmadi-Erber Sarah1,Deutschmann Daniela1,Grigoriev Tetiana2,Chu Ruth2,Leung Cleo2,Tomkinson Adrian2,Uddin Mohammad Nizam3,Moshkani Safiehkhatoon3,Robek Michael D3,Perry Jason2,Lauterbach Henning1,Orlinger Klaus1,Fletcher Simon P2,Balsitis Scott2

Affiliation:

1. Hookipa Pharma , New York, New York , USA

2. Gilead Sciences , Foster City, California , USA

3. Department of Immunology and Microbial Disease, Albany Medical College , Albany, New York , USA

Abstract

Abstract Hepatitis B Virus (HBV) is a major driver of infectious disease mortality. Curative therapies are needed and ideally should induce CD8 T cell-mediated clearance of infected hepatocytes plus anti-hepatitis B surface antigen (HBsAg) antibodies (anti-HBs) to neutralize residual virus. We developed a novel therapeutic vaccine using non-replicating arenavirus vectors. Antigens were screened for genotype conservation and magnitude and genotype reactivity of T cell response, then cloned into Pichinde virus (PICV) vectors (recombinant PICV, GS-2829) and lymphocytic choriomeningitis virus (LCMV) vectors (replication-incompetent, GS-6779). Alternating immunizations with GS-2829 and GS-6779 induced high-magnitude HBV T cell responses, and high anti-HBs titers. Dose schedule optimization in macaques achieved strong polyfunctional CD8 T cell responses against core, HBsAg, and polymerase and high titer anti-HBs. In AAV-HBV mice, GS-2829 and GS-6779 were efficacious in animals with low pre-treatment serum HBsAg. Based on these results, GS-2829 and GS-6779 could become a central component of cure regimens.

Funder

Gilead Sciences

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Immunology and Allergy

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