Impact of Early Versus Late Antiretroviral Treatment Initiation on Naive T Lymphocytes in HIV-1-Infected Children and Adolescents – The-ANRS-EP59-CLEAC Study

Pierre Frange; Pierre Frange; Pierre Frange; Thomas Montange; Thomas Montange; Jérôme Le Chenadec; Damien Batalie; Damien Batalie; Ingrid Fert; Ingrid Fert; Catherine Dollfus; Albert Faye; Stéphane Blanche; Anne Chacé; Corine Fourcade; Isabelle Hau; Martine Levine; Nizar Mahlaoui; Valérie Marcou; Marie-Dominique Tabone; Florence Veber; Alexandre Hoctin; Thierry Wack; Véronique Avettand-Fenoël; Véronique Avettand-Fenoël; Josiane Warszawski; Josiane Warszawski; Florence Buseyne; Florence Buseyne

doi:10.3389/fimmu.2021.662894

Frontiers in Immunology (Apr 2021)

Impact of Early Versus Late Antiretroviral Treatment Initiation on Naive T Lymphocytes in HIV-1-Infected Children and Adolescents – The-ANRS-EP59-CLEAC Study

Pierre Frange,
Pierre Frange,
Pierre Frange,
Thomas Montange,
Thomas Montange,
Jérôme Le Chenadec,
Damien Batalie,
Damien Batalie,
Ingrid Fert,
Ingrid Fert,
Catherine Dollfus,
Albert Faye,
Stéphane Blanche,
Anne Chacé,
Corine Fourcade,
Isabelle Hau,
Martine Levine,
Nizar Mahlaoui,
Valérie Marcou,
Marie-Dominique Tabone,
Florence Veber,
Alexandre Hoctin,
Thierry Wack,
Véronique Avettand-Fenoël,
Véronique Avettand-Fenoël,
Josiane Warszawski,
Josiane Warszawski,
Florence Buseyne,
Florence Buseyne

Affiliations

Pierre Frange: Immunologie, hématologie et rhumatologie pédiatrique, hôpital Necker–Enfants malades, AP–HP- Centre – Université de Paris, Paris, France
Pierre Frange: Laboratoire de microbiologie clinique, hôpital Necker–Enfants malades, AP–HP-Centre – Université de Paris, Paris, France
Pierre Frange: EHU 7328 PACT, Institut Imagine, Université de Paris, Paris, France
Thomas Montange: Unité Epidémiologie et Physiopathologie des Virus Oncogènes, Institut Pasteur, Paris, France
Thomas Montange: Département de Virologie, UMR CNRS 3569 Institut Pasteur, Paris, France
Jérôme Le Chenadec: Départment d’épidémiologie, Centre de Recherche en Épidémiologie et Santé des Populations, INSERM U1018, Le Kremlin-Bicêtre, Villejuif, France
Damien Batalie: Unité Epidémiologie et Physiopathologie des Virus Oncogènes, Institut Pasteur, Paris, France
Damien Batalie: Département de Virologie, UMR CNRS 3569 Institut Pasteur, Paris, France
Ingrid Fert: Unité Epidémiologie et Physiopathologie des Virus Oncogènes, Institut Pasteur, Paris, France
Ingrid Fert: Département de Virologie, UMR CNRS 3569 Institut Pasteur, Paris, France
Catherine Dollfus: Hémato-oncologie pédiatrique, Hôpital Trousseau, AP-HP, Paris, France
Albert Faye: Pédiatrie Générale, Hôpital Robert Debré, AP-HP, Paris, France
Stéphane Blanche: Immunologie, hématologie et rhumatologie pédiatrique, hôpital Necker–Enfants malades, AP–HP- Centre – Université de Paris, Paris, France
Anne Chacé: Pédiatrie et néonatologie, Centre hospitalier intercommunal de Villeuneuve-Saint-Georges, Villeuneuve-Saint-Georges, France
Corine Fourcade: 0Pédiatrie Générale, Hôpital Bicêtre, AP-HP, Paris, France
Isabelle Hau: 1Pédiatrie Générale, Centre hospitalier intercommunal de Créteil, Créteil, France
Martine Levine: 2Immuno-hématologie pédiatrique, Hôpital Robert Debré, AP-HP, Paris, France
Nizar Mahlaoui: Immunologie, hématologie et rhumatologie pédiatrique, hôpital Necker–Enfants malades, AP–HP- Centre – Université de Paris, Paris, France
Valérie Marcou: 3Médecine et réanimation néonatale, Hôpital Cochin, AP-HP-Centre – Université de Paris, Paris, France
Marie-Dominique Tabone: Hémato-oncologie pédiatrique, Hôpital Trousseau, AP-HP, Paris, France
Florence Veber: Immunologie, hématologie et rhumatologie pédiatrique, hôpital Necker–Enfants malades, AP–HP- Centre – Université de Paris, Paris, France
Alexandre Hoctin: Départment d’épidémiologie, Centre de Recherche en Épidémiologie et Santé des Populations, INSERM U1018, Le Kremlin-Bicêtre, Villejuif, France
Thierry Wack: Départment d’épidémiologie, Centre de Recherche en Épidémiologie et Santé des Populations, INSERM U1018, Le Kremlin-Bicêtre, Villejuif, France
Véronique Avettand-Fenoël: Laboratoire de microbiologie clinique, hôpital Necker–Enfants malades, AP–HP-Centre – Université de Paris, Paris, France
Véronique Avettand-Fenoël: 4CNRS 8104/INSERM U1016, Institut Cochin, Université Paris Descartes, Paris, France
Josiane Warszawski: Départment d’épidémiologie, Centre de Recherche en Épidémiologie et Santé des Populations, INSERM U1018, Le Kremlin-Bicêtre, Villejuif, France
Josiane Warszawski: 5INED, Université Paris Sud, Le Kremlin-Bicêtre, Orsay, France
Florence Buseyne: Unité Epidémiologie et Physiopathologie des Virus Oncogènes, Institut Pasteur, Paris, France
Florence Buseyne: Département de Virologie, UMR CNRS 3569 Institut Pasteur, Paris, France

DOI: https://doi.org/10.3389/fimmu.2021.662894
Journal volume & issue: Vol. 12

Abstract

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BackgroundThe early initiation of antiretroviral therapy (ART) in HIV-1-infected infants reduces mortality and prevents early CD4 T-cell loss. However, the impact of early ART on the immune system has not been thoroughly investigated in children over five years of age or adolescents. Here, we describe the levels of naive CD4 and CD8 T lymphocytes (CD4/CD8TN), reflecting the quality of immune reconstitution, as a function of the timing of ART initiation (early (<6 months) versus late (≥24 months of age)).MethodsThe ANRS-EP59-CLEAC study enrolled 27 children (5-12 years of age) and nine adolescents (13-17 years of age) in the early-treatment group, and 19 children (L-Ch) and 21 adolescents (L-Ado) in the late-treatment group. T lymphocytes were analyzed by flow cytometry and plasma markers were analyzed by ELISA. Linear regression analysis was performed with univariate and multivariate models.ResultsAt the time of evaluation, all patients were on ART and had a good immunovirological status: 83% had HIV RNA loads below 50 copies/mL and the median CD4 T-cell count was 856 cells/µL (interquartile range: 685-1236 cells/µL). In children, early ART was associated with higher CD8TN percentages (medians: 48.7% vs. 31.0%, P = 0.001), and a marginally higher CD4TN (61.2% vs. 53.1%, P = 0.33). In adolescents, early ART was associated with low CD4TN percentages and less differentiated memory CD8 T cells. CD4TN and CD8TN levels were inversely related to cellular activation and gut permeability.ConclusionIn children and adolescents, the benefits of early ART for CD8TN were clear after long-term ART. The impact of early ART on CD4TN appears to be modest, because pediatric patients treated late respond to HIV-driven CD4 T-lymphocyte loss by the de novo production of TN cells in the thymus. Our data also suggest that current immune activation and/or gut permeability has a negative impact on TN levels.Clinical Trial RegistrationClinicalTrials.gov, identifier NCT02674867.

Published in Frontiers in Immunology

ISSN: 1664-3224 (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: http://journal.frontiersin.org/journal/immunology

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