Hyperfunctional T cell responses unchecked by regulatory T cells are unable to resolve hepaciviral infection without humoral contribution

IF 26.8 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY Journal of Hepatology Pub Date : 2024-10-17 DOI:10.1016/j.jhep.2024.10.012
Fengzhi Jin, John Gridley, Anuradha Kumari, Alireza Saeidi, Brantley Holland, Elizabeth Elrod, Piyush Dravid, Sheetal Trivedi, Amit Kapoor, Manoj Thapa, Arash Grakoui
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Abstract

Background & Aims

The most recent T cell-based vaccine against hepatitis C virus (HCV) in human subjects failed to swing the pendulum from chronicity to resolution despite eliciting cellular responses in the majority of individuals. These results naturally evoke the question of whether hyperactivated responses of a single adaptive immune arm are capable of inducing HCV clearance or if coordinated efforts between antibodies and T cells are indeed necessary. Here, we sought to address this point in determining whether the suppression of antiviral T cell and IgG responses by regulatory T cells (Tregs) is a critical prerequisite of delayed viral clearance or overt chronicity.

Methods

Using a surrogate model of HCV infection, rodent hepacivirus (RHV) infection in mice, we utilized Foxp3-DTR mice to assess how Tregs modulate the generation of acute antiviral adaptive immune responses and indirectly dictate infection fate via intracellular flow cytometry staining, ELISA, RNA sequencing, and qPCR.

Results

Transient depletion of Tregs prior to infection decreased viral-specific CD4+ T cell function, IgG production, and delayed viral clearance. In contrast, transient Treg depletion after infection increased both T cell functionality and IgG production, thereby facilitating accelerated viral clearance. Hyperactivated T cells, achieved via transient Treg depletion, were unable to clear the virus as an isolated effector arm without the help of viral-specific IgG production.

Conclusions

Tregs control the outcome of RHV infection via direct modulation of CD4+ T cells and IgG production. Hyperactivated T cell responses are incapable of compensating for experimentally induced lack of antibodies, further reinforcing the notion of cooperative interplay between adaptive immune arms in facilitating hepaciviral clearance.

Impact and implications

We demonstrate herein how timing of Treg depletion determines the fate of effector T cells, humoral responses, and the kinetics of viral clearance. Our observations provide direct evidence that functional T cell responses are incapable of compensating for suboptimal humoral responses in facilitating viral resolution. Our results imply that future HCV vaccine regimens should not solely rely on eliciting focused responses of a single effector arm, but rather incorporate immunogens capable of inducing durable features of both humoral and cellular memory.

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功能亢进的 T 细胞反应如果不受调节性 T 细胞的控制,就无法在没有体液贡献的情况下解决肝炎病毒感染问题
背景& 目的最近在人类受试者中使用的基于 T 细胞的丙型肝炎病毒(HCV)疫苗,尽管在大多数个体中引起了细胞反应,但却未能将钟摆从慢性转为清除。这些结果自然而然地引发了一个问题:是单一适应性免疫臂的过度激活反应能够诱导 HCV 清除,还是抗体和 T 细胞之间的协调努力确实是必要的。在此,我们试图解决这个问题,确定调节性 T 细胞(Tregs)抑制抗病毒 T 细胞和 IgG 反应是否是延迟病毒清除或明显慢性化的关键先决条件。方法利用HCV感染的替代模型--小鼠啮齿类肝病毒(RHV)感染,我们利用Foxp3-DTR小鼠评估了调节性Treg如何调节急性抗病毒适应性免疫反应的产生,并通过细胞内流式细胞仪染色、ELISA、RNA测序和qPCR间接决定感染命运。与此相反,感染后一过性Treg耗竭可增加T细胞功能和IgG生成,从而促进病毒清除加速。结论Tregs通过直接调节CD4+ T细胞和IgG的产生来控制RHV感染的结果。超活化的 T 细胞反应无法弥补实验诱导的抗体缺乏,这进一步加强了适应性免疫臂在促进肝病毒清除过程中相互合作的概念。我们的观察结果提供了直接证据,证明功能性 T 细胞反应无法弥补体液反应在促进病毒清除方面的不足。我们的研究结果表明,未来的 HCV 疫苗方案不应仅仅依赖于激发单一效应臂的集中反应,而应结合能够诱导体液和细胞记忆持久特征的免疫原。
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来源期刊
Journal of Hepatology
Journal of Hepatology 医学-胃肠肝病学
CiteScore
46.10
自引率
4.30%
发文量
2325
审稿时长
30 days
期刊介绍: The Journal of Hepatology is the official publication of the European Association for the Study of the Liver (EASL). It is dedicated to presenting clinical and basic research in the field of hepatology through original papers, reviews, case reports, and letters to the Editor. The Journal is published in English and may consider supplements that pass an editorial review.
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