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在抗逆转录病毒治疗抑制的 HIV 感染期间,Vδ1 效应器和 Vδ2 γδ T 细胞亚群的频率发生变化,并与血浆炎症标志物相关。

Vδ1 Effector and Vδ2 γδ T-Cell Subsets Shift in Frequency and Are Linked to Plasma Inflammatory Markers During Antiretroviral Therapy-Suppressed HIV Infection.

机构信息

Department of Medicine, Boston University Chobanian and Avedisian School of Medicine, Boston, Massachusetts, USA.

Department of Virology, Immunology, and Microbiology, Boston University Chobanian and Avedisian School of Medicine, Boston, Massachusetts, USA.

出版信息

J Infect Dis. 2024 May 15;229(5):1317-1327. doi: 10.1093/infdis/jiae091.

DOI:10.1093/infdis/jiae091
PMID:38390982
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11095541/
Abstract

BACKGROUND

Chronic inflammation is prevalent with antiretroviral therapy (ART)-suppressed human immunodeficiency virus (HIV) infection and one immune cell subset putatively driving this phenomenon is TIGIT+ γδ T cells.

METHODS

To elucidate γδ T-cell phenotypic diversity, spectral flow cytometry was performed on blood lymphocytes from individuals of a HIV and aging cohort and data were analyzed using bioinformatic platforms. Plasma inflammatory markers were measured and correlated with γδ T-cell subset frequencies.

RESULTS

Thirty-nine distinct γδ T-cell subsets were identified (22 Vδ1+, 14 Vδ2+, and 3 Vδ1-Vδ2-Vγ9+) and TIGIT was nearly exclusively found on the Vδ1+CD45RA+CD27- effector populations. People with ART-suppressed HIV infection (PWH) exhibited high frequencies of distinct clusters of Vδ1+ effectors distinguished via CD8, CD16, and CD38 expression. Among Vδ2+ cells, most Vγ9+ (innate-like) clusters were lower in PWH; however, CD27+ subsets were similar in frequency between participants with and without HIV. Comparisons by age revealed lower 'naive' Vδ1+CD45RA+CD27+ cells in older individuals, regardless of HIV status. Plasma inflammatory markers were selectively linked to subsets of Vδ1+ and Vδ2+ cells.

CONCLUSIONS

These results further elucidate γδ T-cell subset complexity and reveal distinct alterations and connections with inflammatory pathways of Vδ1+ effector and Vδ2+ innate-like subsets during ART-suppressed HIV infection.

摘要

背景

慢性炎症在接受抗逆转录病毒疗法(ART)抑制的人类免疫缺陷病毒(HIV)感染中很常见,一种被认为是驱动这种现象的免疫细胞亚群是 TIGIT+γδ T 细胞。

方法

为了阐明 γδ T 细胞的表型多样性,对 HIV 和衰老队列个体的血液淋巴细胞进行了光谱流式细胞术检测,并使用生物信息学平台对数据进行了分析。测量了血浆炎症标志物,并将其与 γδ T 细胞亚群频率相关联。

结果

鉴定出 39 种不同的 γδ T 细胞亚群(22 种 Vδ1+、14 种 Vδ2+和 3 种 Vδ1-Vδ2-Vγ9+),TIGIT 几乎仅存在于 Vδ1+CD45RA+CD27-效应细胞群上。接受 ART 抑制的 HIV 感染(PWH)个体表现出高频率的不同 Vδ1+效应细胞簇,这些细胞簇通过 CD8、CD16 和 CD38 的表达来区分。在 Vδ2+细胞中,大多数 Vγ9+(先天样)簇在 PWH 中较低;然而,CD27+亚群在 HIV 阳性和阴性参与者中的频率相似。按年龄比较显示,无论 HIV 状态如何,年龄较大的个体中“幼稚”的 Vδ1+CD45RA+CD27+细胞较低。血浆炎症标志物与 Vδ1+和 Vδ2+细胞亚群选择性相关联。

结论

这些结果进一步阐明了 γδ T 细胞亚群的复杂性,并揭示了在接受 ART 抑制的 HIV 感染期间,Vδ1+效应和 Vδ2+先天样亚群与炎症途径的独特改变和关联。