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. 2024 Dec;57(6):854-867.
doi: 10.1016/j.jmii.2024.08.007. Epub 2024 Aug 22.

The persistence of low CD4/CD8 ratio in chronic HIV-infection, despite ART suppression and normal CD4 levels, is associated with pre-therapy values of inflammation and thymic function

Vanesa Garrido-Rodríguez  1 Ángel Bulnes-Ramos  2 Israel Olivas-Martínez  3 María Del Mar Pozo-Balado  4 Ana Isabel Álvarez-Ríos  5 Félix Gutiérrez  6 Rebeca Izquierdo  7 Federico García  8 Juan Manuel Tiraboschi  9 Francisco Vera-Méndez  10 Joaquim Peraire  11 Anna Rull  12 Yolanda María Pacheco  13 CoRIS cohort
Affiliations
Free article

The persistence of low CD4/CD8 ratio in chronic HIV-infection, despite ART suppression and normal CD4 levels, is associated with pre-therapy values of inflammation and thymic function

Vanesa Garrido-Rodríguez et al. J Microbiol Immunol Infect. 2024 Dec.
Free article

Abstract

Background: Persistence of a low CD4/CD8 ratio is associated with an increased morbimortality in people living with HIV (PLWH) under effective antiretroviral therapy. We aimed to explore the immunological significance of a persistently low CD4/CD8 ratio, even despite normal CD4 levels, and assess whether these features vary from those associated to a low nadir-CD4, another well-established predictor of disease progression.

Methods: CD4-recovered PLWH were classified by CD4/CD8 ratio after three-years of ART (viral suppression, CD4≥500; R < 0.8, n = 24 and R > 1.2, n = 28). sj/β-TRECs ratio and inflammatory-related markers were quantified. PBMCs were immunophenotyped by CyTOF and functionally characterized by ELISPOT. Subjects were also reclassified depending on nadir-CD4 (N ≤ 350/N > 350).

Results: R < 0.8 showed a differential inflammatory profile compared to R > 1.2 (increased β2-microglobulin, D-dimers and IP-10 before ART). R < 0.8 presented lower baseline thymic function, being inversely correlated with post-ART inflammation. R < 0.8 at follow-up showed most alterations in CD8 subsets (increasing frequency and exhibiting a senescent phenotype [e.g., CD57+, CD95+]) and enhanced T-cell IFNγ/IL-2 secretion. However, comparing N ≤ 350 to N > 350, the main features were altered functional markers in CD4 T-cells, despite no differences in maturational subsets, together with a restricted T-cell cytokine secretion pattern.

Conclusion: Persistence of low CD4/CD8 ratio in successfully-treated PLWH, with normal CD4 counts, is associated with baseline inflammation and low thymic function, and it features post-therapy alterations specific to CD8 T-cells. Differently, subjects recovered from low nadir-CD4 in this setting feature post-therapy alterations on CD4 T-cells. Hence, different mechanisms of disease progression could underlie these biomarkers, potentially requiring different clinical approaches.

Keywords: CD4/CD8 ratio; HIV-Infection; Immunological dysfunction; Nadir-CD4 T-cell; sj/β-TRECs.

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Conflict of interest statement

Declaration of competing interest The authors declare that they have no conflicts of interest.