Early antiretroviral therapy favors post-treatment SIV control associated with the expansion of enhanced memory CD8+ T-cells

Author:

Passaes CarolineORCID,Desjardins DelphineORCID,Chapel Anaïs,Monceaux ValérieORCID,Lemaitre Julien,Mélard AdelineORCID,Perdomo-Celis FedericoORCID,Planchais CyrilORCID,Gourvès MaëlORCID,Dimant NastasiaORCID,David Annie,Dereuddre-Bosquet NathalieORCID,Barrail-Tran AurélieORCID,Gouget Hélène,Guillaume Céline,Relouzat FrancisORCID,Lambotte Olivier,Guedj JérémieORCID,Müller-Trutwin MichaelaORCID,Mouquet HugoORCID,Rouzioux Christine,Avettand-Fenoël VéroniqueORCID,Le Grand RogerORCID,Sáez-Cirión AsierORCID

Abstract

AbstractHIV remission can be achieved in some people, called post-treatment HIV controllers, after antiretroviral treatment discontinuation. Treatment initiation close to the time of infection was suggested to favor post-treatment control, but the circumstances and mechanisms leading to this outcome remain unclear. Here we evaluate the impact of early (week 4) vs. late (week 24 post-infection) treatment initiation in SIVmac251-infected male cynomolgus macaques receiving 2 years of therapy before analytical treatment interruption. We show that early treatment strongly promotes post-treatment control, which is not related to a lower frequency of infected cells at treatment interruption. Rather, early treatment favors the development of long-term memory CD8+ T cells with enhanced proliferative and SIV suppressive capacity that are able to mediate a robust secondary-like response upon viral rebound. Our model allows us to formally demonstrate a link between treatment initiation during primary infection and the promotion of post-treatment control and provides results that may guide the development of new immunotherapies for HIV remission.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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