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

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Listed:
  • Caroline Passaes

    (Université Paris Cité, Viral Reservoirs and Immune Control Unit
    Université Paris Cité, HIV Inflammation and Persistence Unit)

  • Delphine Desjardins

    (Université Paris-Saclay, CEA, INSERM, UMR1184, Immunology of Viral, Auto-immune, Hematological and Bacterial diseases (IMVA-HB/IDMIT Department))

  • Anaïs Chapel

    (Université Paris Cité, Viral Reservoirs and Immune Control Unit
    Université Paris Cité, HIV Inflammation and Persistence Unit)

  • Valérie Monceaux

    (Université Paris Cité, Viral Reservoirs and Immune Control Unit
    Université Paris Cité, HIV Inflammation and Persistence Unit)

  • Julien Lemaitre

    (Université Paris-Saclay, CEA, INSERM, UMR1184, Immunology of Viral, Auto-immune, Hematological and Bacterial diseases (IMVA-HB/IDMIT Department))

  • Adeline Mélard

    (Université Paris Cité; INSERM, U1016; CNRS)

  • Federico Perdomo-Celis

    (Université Paris Cité, HIV Inflammation and Persistence Unit)

  • Cyril Planchais

    (Institut Pasteur, Université Paris Cité, INSERM U1222, Humoral Immunology Unit)

  • Maël Gourvès

    (Université Paris Cité, Viral Reservoirs and Immune Control Unit)

  • Nastasia Dimant

    (Université Paris-Saclay, CEA, INSERM, UMR1184, Immunology of Viral, Auto-immune, Hematological and Bacterial diseases (IMVA-HB/IDMIT Department))

  • Annie David

    (Université Paris Cité, HIV Inflammation and Persistence Unit)

  • Nathalie Dereuddre-Bosquet

    (Université Paris-Saclay, CEA, INSERM, UMR1184, Immunology of Viral, Auto-immune, Hematological and Bacterial diseases (IMVA-HB/IDMIT Department))

  • Aurélie Barrail-Tran

    (Université Paris-Saclay, CEA, INSERM, UMR1184, Immunology of Viral, Auto-immune, Hematological and Bacterial diseases (IMVA-HB/IDMIT Department)
    Université Paris-Saclay, AP-HP, Hôpital Bicêtre, Service de Pharmacie)

  • Hélène Gouget

    (Université Paris-Saclay, CEA, INSERM, UMR1184, Immunology of Viral, Auto-immune, Hematological and Bacterial diseases (IMVA-HB/IDMIT Department))

  • Céline Guillaume

    (Université Paris-Saclay, CEA, INSERM, UMR1184, Immunology of Viral, Auto-immune, Hematological and Bacterial diseases (IMVA-HB/IDMIT Department))

  • Francis Relouzat

    (Université Paris-Saclay, CEA, INSERM, UMR1184, Immunology of Viral, Auto-immune, Hematological and Bacterial diseases (IMVA-HB/IDMIT Department))

  • Olivier Lambotte

    (Université Paris-Saclay, CEA, INSERM, UMR1184, Immunology of Viral, Auto-immune, Hematological and Bacterial diseases (IMVA-HB/IDMIT Department)
    Université Paris-Saclay, AP-HP. Hôpital Bicêtre, Clinical Immunology Department)

  • Jérémie Guedj

    (Université Paris Cité, IAME, INSERM)

  • Michaela Müller-Trutwin

    (Université Paris Cité, HIV Inflammation and Persistence Unit)

  • Hugo Mouquet

    (Institut Pasteur, Université Paris Cité, INSERM U1222, Humoral Immunology Unit)

  • Christine Rouzioux

    (Université Paris Cité/APHP Hôpital Necker - Enfants Malades)

  • Véronique Avettand-Fenoël

    (Université Paris Cité; INSERM, U1016; CNRS
    APHP Hôpital Cochin, Service de Virologie)

  • Roger Le Grand

    (Université Paris-Saclay, CEA, INSERM, UMR1184, Immunology of Viral, Auto-immune, Hematological and Bacterial diseases (IMVA-HB/IDMIT Department))

  • Asier Sáez-Cirión

    (Université Paris Cité, Viral Reservoirs and Immune Control Unit
    Université Paris Cité, HIV Inflammation and Persistence Unit)

Abstract

HIV 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.

Suggested Citation

  • Caroline Passaes & Delphine Desjardins & Anaïs Chapel & Valérie Monceaux & Julien Lemaitre & Adeline Mélard & Federico Perdomo-Celis & Cyril Planchais & Maël Gourvès & Nastasia Dimant & Annie David & , 2024. "Early antiretroviral therapy favors post-treatment SIV control associated with the expansion of enhanced memory CD8+ T-cells," Nature Communications, Nature, vol. 15(1), pages 1-19, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-023-44389-3
    DOI: 10.1038/s41467-023-44389-3
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    References listed on IDEAS

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