慢性HCV感染促进抗原特异性CD8+T细胞的细胞毒性,而与病毒特异性无关

IF 2 Q4 VIROLOGY
Ana C. Maretti‐Mira, M. Salomon, Angela M. Hsu, C. Matsuba, L. Golden‐Mason
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摘要

引言尽管丙型肝炎病毒(HCV)感染治疗取得了进展,但HCV仍然是一个重大的公共卫生负担。除了进行性肝损伤外,病毒的持久性对先天和适应性免疫反应也有持久的影响。缺乏对驱动有效HCV反应的因素的完全理解导致了未能开发出预防疫苗。本研究推进了对HCV特异性CD8+T细胞的现有知识,并描述了当前或过去HCV感染对其他病毒特异性CD8+T细胞的影响。方法我们使用条形码右旋支架对HCV、巨细胞病毒和流感特异性CD8+T细胞进行鉴定和分类,并使用单细胞RNA测序技术对其进行表征。我们的队列包括慢性(cHCV)、自发消退(rHCV)和接受直接作用抗病毒(DAA)治疗的受试者。结果我们发现丙型肝炎病毒特异性CD8+T细胞在cHCV患者中具有细胞毒性特征,DAA治疗后细胞毒性逐渐减少,并在治疗完成后持续12周。我们还观察到,在DAA治疗中,CD8+T细胞表型发生了变化,效应记忆降低,细胞信号耗尽。在rHCV中,与cHCV相比,我们还检测到较小比例的效应记忆细胞。cHCV和rHCV受试者中CD8+耗竭的T细胞比例相当。此外,我们还观察到非HCV病毒特异性CD8+T细胞在cHCV感染期间表现出强大的细胞毒性特征。总之,我们的研究结果表明,无论病毒特异性如何,cHCV感染都能促进CD8+T细胞的细胞毒性。CD8+T细胞中由cHCV感染引起的免疫变化可能有助于恶化HCV感染造成的持续肝损伤,或加剧对可能的合并感染的免疫反应。我们的数据为探索丙型肝炎病毒特异性T细胞自发和治疗诱导消退的潜在机制的小组提供了资源,为开发有效的丙型肝炎病毒感染疫苗提供了信息。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Chronic HCV infection promotes cytotoxicity in antigen-specific CD8+ T cells regardless of virus specificity
Introduction Despite advancements in hepatitis C virus (HCV) infection treatment, HCV still represents a significant public health burden. Besides progressive hepatic damage, viral persistence has lasting effects on innate and adaptive immune responses. Lack of a complete understanding of the factors driving an effective HCV response contributes to the failure to develop a vaccine for prevention. This study advances the existing knowledge on HCV-specific CD8+ T cells and describes the impact of current or past HCV infection on CD8+ T cells specific for other viruses. Methods We used barcoded-dextramers to identify and sort CD8+ T cells specific for HCV, cytomegalovirus, and influenza, and characterized them using single-cell RNA sequencing technology. Our cohort included chronic (cHCV), spontaneously resolved (rHCV), and subjects undergoing direct-acting antiviral (DAA) therapy. Results We show that HCV-specific CD8+ T cells have cytotoxic features in patients with cHCV, which is progressively reduced with DAA therapy and persists 12 weeks after treatment completion. We also observe a shift in the CD8+ T cell phenotype on DAA treatment, with decreased effector memory and exhausted cell signatures. In rHCV, we also detected a smaller proportion of effector memory cells compared to cHCV. The proportion of CD8+ exhausted T cells in cHCV and rHCV subjects was comparable. Moreover, we also observed that non-HCV virus-specific CD8+ T cells exhibit robust cytotoxic traits during cHCV infection. Discussion Altogether, our findings suggest that cHCV infection promotes cytotoxicity in CD8+ T cells regardless of virus specificity. The immunological changes caused by cHCV infection in CD8+ T cells may contribute to worsening the ongoing hepatic damage caused by HCV infection or exacerbate the immune response to possible co-infections. Our data provide a resource to groups exploring the underlying mechanisms of HCV-specific T cell spontaneous and treatment-induced resolution to inform the development of effective vaccines against HCV infection.
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