[HTML][HTML] Mosaic HIV-1 vaccines expand the breadth and depth of cellular immune responses in rhesus monkeys

DH Barouch, KL O'brien, NL Simmons, SL King… - Nature medicine, 2010 - nature.com
DH Barouch, KL O'brien, NL Simmons, SL King, P Abbink, LF Maxfield, YH Sun, A La Porte…
Nature medicine, 2010nature.com
The worldwide diversity of HIV-1 presents an unprecedented challenge for vaccine
development,. Antigens derived from natural HIV-1 sequences have elicited only a limited
breadth of cellular immune responses in nonhuman primate studies and clinical trials to
date. Polyvalent'mosaic'antigens, in contrast, are designed to optimize cellular immunologic
coverage of global HIV-1 sequence diversity. Here we show that mosaic HIV-1 Gag, Pol and
Env antigens expressed by recombinant, replication-incompetent adenovirus serotype 26 …
Abstract
The worldwide diversity of HIV-1 presents an unprecedented challenge for vaccine development,. Antigens derived from natural HIV-1 sequences have elicited only a limited breadth of cellular immune responses in nonhuman primate studies and clinical trials to date. Polyvalent 'mosaic' antigens, in contrast, are designed to optimize cellular immunologic coverage of global HIV-1 sequence diversity. Here we show that mosaic HIV-1 Gag, Pol and Env antigens expressed by recombinant, replication-incompetent adenovirus serotype 26 vectors markedly augmented both the breadth and depth without compromising the magnitude of antigen-specific T lymphocyte responses as compared with consensus or natural sequence HIV-1 antigens in rhesus monkeys. Polyvalent mosaic antigens therefore represent a promising strategy to expand cellular immunologic vaccine coverage for genetically diverse pathogens such as HIV-1.
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