通过增强 miRNA-30b、30c 和 30e，升高的 ATP 下调 HIV 感染个体 CD8+ T 细胞中 CD73 的表达。

Elevated ATP via enhanced miRNA-30b, 30c, and 30e downregulates the expression of CD73 in CD8+ T cells of HIV-infected individuals.

机构信息

School of Dentistry, Division of Foundational Sciences, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, Canada.

Department of Medicine, Division of Neurology, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, Canada.

出版信息

PLoS Pathog. 2022 Mar 24;18(3):e1010378. doi: 10.1371/journal.ppat.1010378. eCollection 2022 Mar.

DOI:10.1371/journal.ppat.1010378

PMID:35325005

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8947394/

Abstract

CD8+ T cells play a crucial role against chronic viral infections, however, their effector functions are influenced by the expression of co-stimulatory/inhibitory receptors. For example, CD73 works with CD39 to convert highly inflammatory ATP to adenosine. However, its expression on T cells in the context of viral infections has not been well defined. Here, we analyzed the expression of CD73 on human T cells in a cohort of 102 HIV-infected individuals including those on antiretroviral therapy (ART), ART-naïve, and long-term non-progressors who were not on ART. We found that the frequency of CD73+ T cells was markedly lower among T cell subsets (e.g. naïve, effector or memory) in the peripheral blood of all HIV-infected individuals. Notably, CD73 was decreased at the cell surface, intracellular and gene levels. Functionally, CD8+CD73+ T cells exhibited decreased cytokine expression (TNF-α, IFN-γ and IL-2) upon global or antigen-specific stimulation and impaired expression of cytolytic molecules at the gene and protein levels. In contrast, CD8+CD73+ T cells expressed elevated levels of homing receptors such as CCR7, α4β7 integrin, which suggests a migratory advantage for these cells as observed in vitro. We also observed significant migration of CD73+CD8+ T cells into the cerebrospinal fluids of multiple sclerosis (MS) patients at the time of disease relapse. Moreover, we found that elevated levels of ATP in the plasma of HIV-infected individuals upregulates the expression of miRNA30b-e in T cells in vitro. In turn, inhibition of miRNAs (30b, 30c and 30e) resulted in significant upregulation of CD73 mRNA in CD8+ T cells. Therefore, we provide a novel mechanism for the downregulation of CD73 via ATP-induced upregulation of miRNA30b, 30c and 30e in HIV infection. Finally, these observations imply that ATP-mediated downregulation of CD73 mainly occurs via its receptor, P2X1/P2RX1. Our results may in part explain why HIV-infected individuals have reduced risk of developing MS considering the role of CD73 for efficient T cell entry into the central nervous system.

摘要

CD8+ T 细胞在对抗慢性病毒感染中起着至关重要的作用，然而，它们的效应功能受到共刺激/抑制受体表达的影响。例如，CD73 与 CD39 一起将高度炎症性的 ATP 转化为腺苷。然而，其在病毒感染中的 T 细胞表达尚未得到很好的定义。在这里，我们分析了 102 名 HIV 感染者（包括接受抗逆转录病毒治疗 (ART)、未接受 ART 的 ART 初治者和长期非进展者）队列中 CD73 在人 T 细胞上的表达。我们发现，所有 HIV 感染者外周血中的 T 细胞亚群（如幼稚、效应或记忆）中 CD73+T 细胞的频率明显降低。值得注意的是，CD73 在细胞表面、细胞内和基因水平上均减少。功能上，CD8+CD73+T 细胞在整体或抗原特异性刺激下细胞因子表达（TNF-α、IFN-γ 和 IL-2）减少，并且在基因和蛋白水平上细胞溶解分子的表达受损。相比之下，CD8+CD73+T 细胞表达高水平的归巢受体，如 CCR7、α4β7 整合素，这表明这些细胞具有迁移优势，如在体外观察到的那样。我们还观察到在多发性硬化症 (MS) 患者疾病复发时，CD73+CD8+T 细胞大量迁移到脑脊液中。此外，我们发现 HIV 感染者血浆中高水平的 ATP 在体外上调 T 细胞中 miRNA30b-e 的表达。反过来，抑制 miRNA（30b、30c 和 30e）导致 CD8+T 细胞中 CD73 mRNA 的显著上调。因此，我们提供了一种新的机制，即 HIV 感染通过 ATP 诱导 miRNA30b、30c 和 30e 的上调来下调 CD73 的表达。最后，这些观察结果表明，ATP 介导的 CD73 下调主要通过其受体 P2X1/P2RX1 发生。我们的结果部分解释了为什么 HIV 感染者患 MS 的风险降低，考虑到 CD73 对 T 细胞有效进入中枢神经系统的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f08d/8947394/2db44b304ae5/ppat.1010378.g001.jpg

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通过增强 miRNA-30b、30c 和 30e，升高的 ATP 下调 HIV 感染个体 CD8+ T 细胞中 CD73 的表达。

Elevated ATP via enhanced miRNA-30b, 30c, and 30e downregulates the expression of CD73 in CD8+ T cells of HIV-infected individuals.

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