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© Research
Publication : NPJ vaccines

A recombinant measles virus vaccine strongly reduces SHIV viremia and virus reservoir establishment in macaques.

Scientific Fields
Diseases
Organisms
Applications
Technique

Published in NPJ vaccines - 22 Oct 2021

Nzounza P, Martin G, Dereuddre-Bosquet N, Najburg V, Gosse L, Ruffié C, Combredet C, Petitdemange C, Souquère S, Schlecht-Louf G, Moog C, Pierron G, Le Grand R, Heidmann T, Tangy F

Link to Pubmed [PMID] – 34686669

Link to DOI – 10.1038/s41541-021-00385-6

NPJ Vaccines 2021 Oct; 6(1): 123

Replicative vectors derived from live-attenuated measles virus (MV) carrying additional non-measles vaccine antigens have long demonstrated safety and immunogenicity in humans despite pre-existing immunity to measles. Here, we report the vaccination of cynomolgus macaques with MV replicative vectors expressing simian-human immunodeficiency virus Gag, Env, and Nef antigens (MV-SHIV Wt) either wild type or mutated in the immunosuppressive (IS) domains of Nef and Env antigens (MV-SHIV Mt). We found that the inactivation of Nef and Env IS domains by targeted mutations led to the induction of significantly enhanced post-prime cellular immune responses. After repeated challenges with low doses of SHIV-SF162p3, vaccinees were protected against high viremia, resulting in a 2-Log reduction in peak viremia, accelerated viral clearance, and a decrease -even complete protection for nearly half of the monkeys- in reservoir cell infection. This study demonstrates the potential of a replicative viral vector derived from the safe and widely used measles vaccine in the development of a future human vaccine against HIV-1.