Jarrett Lopez-Scarim, Dustyn Mendoza, Shashank M Nambiar, Eva Billerbeck
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Early CD4+ T cell help was essential for CD8+ T cell priming and viral clearance, while CD4+ T cells became dispensable during later stages of acute infection. Effector CD8+ T cells directly mediated timely hepacivirus clearance. An analysis of hepatic CD8+ T cells specific for two different viral epitopes revealed the induction of subsets of liver-homing CD103+CD49a+ and CD103-CD49a+ effector CD8+ T cells with elevated IFN-γ and TNF-α production. CD103+CD49a+ T cells further persisted as tissue-resident memory subsets. A lack of CD4+ T cell help and CD40L-CD40 interactions resulted in reduced effector functions and phenotypical changes in effector CD8+ T cells and a specific loss of the CD103+CD49a+ subset. 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引用次数: 0
摘要
在丙型肝炎病毒(HCV)感染中,CD4+和CD8+ T细胞对病毒控制至关重要。然而,目前还缺乏对 CD4+ T 细胞帮助的动力学及其在急性感染期间生成不同 CD8+ T 细胞亚群中的作用的详细了解。小型 HCV 动物模型的缺乏阻碍了肝脏抗病毒 T 细胞免疫的机理研究和 HCV 疫苗的开发。在本研究中,我们利用最近开发的一种 HCV 相关啮齿类动物肝病毒感染小鼠模型,研究了体内肝病毒感染过程中 CD4+ T 细胞对肝 CD8+ T 细胞应答和病毒清除的影响。我们的研究结果揭示了急性感染期间 CD4+ T 细胞依赖性的特定动力学。早期 CD4+ T 细胞的帮助对 CD8+ T 细胞的启动和病毒清除至关重要,而在急性感染的后期,CD4+ T 细胞变得可有可无。效应CD8+ T细胞直接介导肝炎病毒的及时清除。对两种不同病毒表位特异性肝脏 CD8+ T 细胞的分析表明,肝脏归巢 CD103+CD49a+ 和 CD103-CD49a+ 效应 CD8+ T 细胞亚群诱导了 IFN-γ 和 TNF-α 的产生。CD103+CD49a+ T细胞作为组织驻留记忆亚群进一步持续存在。CD4+ T细胞帮助和CD40L-CD40相互作用的缺乏导致效应CD8+ T细胞的效应功能降低、表型改变以及CD103+CD49a+亚群的特异性丧失。总之,我们的研究表明,早期 CD4+ T 细胞通过 CD40L 信号转导提供的帮助对于启动功能性效应 CD8+ T 细胞亚群(包括独特的肝脏归属亚群)和清除肝炎病毒至关重要。
CD4+ T cell help during early acute hepacivirus infection is critical for viral clearance and the generation of a liver-homing CD103+CD49a+ effector CD8+ T cell subset.
In hepatitis C virus (HCV) infection, CD4+ and CD8+ T cells are crucial for viral control. However, a detailed understanding of the kinetic of CD4+ T cell help and its role in the generation of different CD8+ T cell subsets during acute infection is lacking. The absence of a small HCV animal model has impeded mechanistic studies of hepatic antiviral T cell immunity and HCV vaccine development. In this study, we used a recently developed HCV-related rodent hepacivirus infection mouse model to investigate the impact of CD4+ T cell help on the hepatic CD8+ T cell response and viral clearance during hepacivirus infection in vivo. Our results revealed a specific kinetic of CD4+ T cell dependency during acute infection. Early CD4+ T cell help was essential for CD8+ T cell priming and viral clearance, while CD4+ T cells became dispensable during later stages of acute infection. Effector CD8+ T cells directly mediated timely hepacivirus clearance. An analysis of hepatic CD8+ T cells specific for two different viral epitopes revealed the induction of subsets of liver-homing CD103+CD49a+ and CD103-CD49a+ effector CD8+ T cells with elevated IFN-γ and TNF-α production. CD103+CD49a+ T cells further persisted as tissue-resident memory subsets. A lack of CD4+ T cell help and CD40L-CD40 interactions resulted in reduced effector functions and phenotypical changes in effector CD8+ T cells and a specific loss of the CD103+CD49a+ subset. In summary, our study shows that early CD4+ T cell help through CD40L signaling is essential for priming functional effector CD8+ T cell subsets, including unique liver-homing subsets, and hepacivirus clearance.
期刊介绍:
Bacteria, fungi, parasites, prions and viruses cause a plethora of diseases that have important medical, agricultural, and economic consequences. Moreover, the study of microbes continues to provide novel insights into such fundamental processes as the molecular basis of cellular and organismal function.