Arenavirus-Based Vectors Generate Robust SIV Immunity in Non-Human Primates

Author:

Sharma Bhawna1,Bekerman Elena1,Truong Hoa1,Lee Johnny1,Gamez-Guerrero Maria1,Boopathy Archana1,Mital Rohit1ORCID,Huang Katell Bidet2,Ahmadi-Erber Sarah2,Wimmer Raphaela2,Schulha Sophie2,Lauterbach Henning2ORCID,Orlinger Klaus2,Suthram Silpa1,Lewis Mark G.3,Blair Wade1,Makadzange Tariro1ORCID,Geleziunas Romas1,Murry Jeffrey P.1ORCID,Schmidt Sarah2

Affiliation:

1. Gilead Sciences, Inc., Foster City, CA 94404, USA

2. Hookipa Pharma Inc., New York, NY 10018, USA

3. Bioqual, Inc., Rockville, MD 20850, USA

Abstract

Arenavirus-based vectors are being investigated as therapeutic vaccine candidates with the potential to elicit robust CD8 T-cell responses. We compared the immunogenicity of replicating (artPICV and artLCMV) and non-replicating (rPICV and rLCMV) arenavirus-based vectors expressing simian immunodeficiency virus (SIV) Gag and Envelope (Env) immunogens in treatment-naïve non-human primates. Heterologous regimens with non-replicating and replicating vectors elicited more robust SIV IFN-γ responses than a homologous regimen, and replicating vectors elicited significantly higher cellular immunogenicity than non-replicating vectors. The heterologous regimen elicited high anti-Env antibody titers when administered intravenously, with replicating vectors inducing significantly higher titers than non-replicating vectors. Intramuscular immunization resulted in more durable antibody responses than intravenous immunization for both vector platforms, with no difference between the replicating and non-replicating vectors. Overall, both replicating and non-replicating arenavirus vectors generated robust T- and B-cell-mediated immunity to SIV antigens in treatment-naïve non-human primates, supporting further evaluation of these vectors in a clinical setting for HIV therapy.

Funder

Gilead Sciences

Publisher

MDPI AG

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