# HIV Productively Infects Highly Differentiated and Exhausted CD4+ T Cells During AIDS

**Authors:** Clayton Faua, Axel Ursenbach, Anne Fuchs, Stéphanie Caspar, Frédérick Jegou, Yvon Ruch, Baptiste Hoellinger, Elodie Laugel, Aurélie Velay, David Rey, Samira Fafi-Kremer, Pierre Gantner

PMC · DOI: 10.20411/pai.v8i2.638 · Pathogens and Immunity · 2024-02-22

## TL;DR

This study finds that HIV preferentially infects highly differentiated and exhausted CD4+ T cells during AIDS, which may drive viral production and spread in the late stages of infection.

## Contribution

The study identifies the specific CD4+ T cell phenotypes targeted by HIV during AIDS, revealing a shift in infection patterns in advanced disease.

## Key findings

- Productively infected CD4+ T cells during AIDS are more frequently CD4low, HLA-ABClow, CD45RA-, Ki67+, and PD-1+.
- These cells are enriched in memory and exhausted phenotypes and less frequently pTfh-like during AIDS.
- Productively infected cells are skewed toward specific UMAP clusters, indicating preferential targeting of differentiated and exhausted cells.

## Abstract

Throughout HIV infection, productively infected cells generate billions of viral particles and are thus responsible for body-wide HIV dissemination, but their phenotype during AIDS is unknown. As AIDS is associated with immunological changes, analyzing the phenotype of productively infected cells can help understand HIV production during this terminal stage.

Blood samples from 15 untreated viremic participants (recent infection, n=5; long-term infection, n=5; active opportunistic AIDS-defining disease, n=5) and 5 participants virologically controlled on antiretroviral therapy (ART) enrolled in the Analysis of the Persistence, Reservoir and HIV Latency (APRIL) study (NCT05752318) were analyzed. Cells expressing the capsid protein p24 (p24+ cells) after 18 hours of resting or 24 hours of stimulation (HIV-Flow) revealed productively infected cells from viremic participants or translation-competent reservoir cells from treated participants, respectively.

The frequency of productively infected cells tended to be higher during AIDS in comparison with recent and long-term infections (median, 340, 72, and 32/million CD4+ T cells, respectively) and correlated with the plasma viral load at all stages of infection. Altogether, these cells were more frequently CD4low, HLA-ABClow, CD45RA-, Ki67+, PD-1+, with a non-negligible contribution from pTfh (CXCR5+PD-1+) cells, and were not significantly enriched in HIV coreceptors CCR5 nor CXCR4 expression. The comparison markers expression between stages showed that productively infected cells during AIDS were enriched in memory and exhausted cells. In contrast, the frequencies of infected pTfh were lower during AIDS compared to non-AIDS stages. A UMAP analysis revealed that total CD4+ T cells were grouped in 7 clusters and that productive p24+ cells were skewed to given clusters throughout the course of infection. Overall, the preferential targets of HIV during the latest stages seemed to be more frequently highly differentiated (memory, TTD-like) and exhausted cells and less frequently pTfh-like cells. In contrast, translation-competent reservoir cells were less frequent (5/million CD4+ T cells) and expressed more frequently HLA-ABC and less frequently PD-1.

In long-term infection and AIDS, productively infected cells were differentiated and exhausted. This could indicate that cells with these given features are responsible for HIV production and dissemination in an immune dysfunction environment occurring during the last stages of infection.

## Linked entities

- **Proteins:** TMED2 (transmembrane p24 trafficking protein 2), CD4 (CD4 molecule), Mki67 (antigen identified by monoclonal antibody Ki 67), PDCD1 (programmed cell death 1), CXCR5 (C-X-C motif chemokine receptor 5)
- **Diseases:** AIDS (MONDO:0012268)

## Full-text entities

- **Genes:** CXCR5 (C-X-C motif chemokine receptor 5) [NCBI Gene 643] {aka BLR1, CD185, MDR15}, CD4 (CD4 molecule) [NCBI Gene 920] {aka CD4mut, IMD79, Leu-3, OKT4D, T4}, PTPRC (protein tyrosine phosphatase receptor type C) [NCBI Gene 5788] {aka B220, CD45, CD45R, GP180, IMD105, L-CA}, TMED2 (transmembrane p24 trafficking protein 2) [NCBI Gene 10959] {aka P24A, RNP24, p24, p24b1, p24beta1}, CXCR4 (C-X-C motif chemokine receptor 4) [NCBI Gene 7852] {aka CD184, D2S201E, FB22, HM89, HSY3RR, LCR1}, CCR5 (C-C motif chemokine receptor 5) [NCBI Gene 1234] {aka CC-CKR-5, CCCKR5, CCR-5, CD195, CKR-5, CKR5}
- **Diseases:** AIDS (MESH:D000163), infected (MESH:D007239), long-term infection (MESH:D000088562), HIV (MESH:D015658), immune dysfunction (MESH:D007154)
- **Species:** Human immunodeficiency virus 1 (no rank) [taxon 11676]

## Full text

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## Figures

3 figures with captions in the complete paper: https://tomesphere.com/paper/PMC10901154/full.md

## References

53 references — full list in the complete paper: https://tomesphere.com/paper/PMC10901154/full.md

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Source: https://tomesphere.com/paper/PMC10901154