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

Q1 Medicine
Pathogens and Immunity Pub Date : 2024-02-22 eCollection Date: 2023-01-01 DOI:10.20411/pai.v8i2.638
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
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引用次数: 0

Abstract

Background: 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.

Methods: 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.

Results: 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.

Conclusions: 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.

艾滋病期间,艾滋病毒能有效感染高度分化和衰竭的 CD4+ T 细胞。
背景:在艾滋病病毒感染的整个过程中,产生性感染细胞会产生数十亿病毒颗粒,从而负责在全身范围内传播艾滋病病毒,但它们在艾滋病期间的表型尚不清楚。由于艾滋病与免疫学变化有关,分析产生性感染细胞的表型有助于了解艾滋病晚期的 HIV 产生情况:方法:分析了 15 名未接受治疗的病毒感染者(近期感染,5 人;长期感染,5 人;活动性机会性 AIDS 定义疾病,5 人)和 5 名接受抗逆转录病毒疗法(ART)病毒学控制的参与者的血液样本,这些参与者都参加了 "持久性、贮存库和 HIV 潜伏期分析"(APRIL)研究(NCT05752318)。经过 18 小时静息或 24 小时刺激(HIV-Flow)后表达囊状蛋白 p24 的细胞(p24+ 细胞)分别显示了来自病毒携带者的生产性感染细胞或来自接受治疗者的具有翻译能力的储库细胞:结果:与近期感染和长期感染相比,艾滋病期间生产性感染细胞的频率往往更高(中位数分别为 340、72 和 32 个/百万 CD4+ T 细胞),并且在感染的各个阶段都与血浆病毒载量相关。总之,这些细胞更常见的是CD4-low、HLA-ABC-low、CD45RA-、Ki67+、PD-1+,其中pTfh(CXCR5+PD-1+)细胞的贡献不可忽略,而且在HIV核心受体CCR5或CXCR4表达方面没有明显富集。不同阶段标志物表达的比较显示,艾滋病期间的生产性感染细胞富含记忆细胞和衰竭细胞。相反,与非艾滋病期相比,艾滋病期感染 pTfh 的频率较低。UMAP 分析显示,CD4+ T 细胞总数分为 7 个群组,而在整个感染过程中,有生产力的 p24+ 细胞向特定群组倾斜。总体而言,在最后期,HIV 的首选目标似乎更多是高分化(记忆、TTD 样)和衰竭细胞,而较少是 pTfh 样细胞。相比之下,翻译能力强的储备细胞出现的频率较低(5/百万 CD4+ T 细胞),表达 HLA-ABC 的频率较高,表达 PD-1 的频率较低:结论:在长期感染和艾滋病中,有生产力的感染细胞被分化和耗竭。这可能表明,在感染的最后阶段,具有这些特征的细胞在免疫功能紊乱的环境中负责艾滋病毒的产生和传播。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Pathogens and Immunity
Pathogens and Immunity Medicine-Infectious Diseases
CiteScore
10.60
自引率
0.00%
发文量
16
审稿时长
10 weeks
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