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急性丙型肝炎的转归与病毒特异性CD4功能及抗病毒记忆性CD8反应的成熟有关。

Outcome of acute hepatitis C is related to virus-specific CD4 function and maturation of antiviral memory CD8 responses.

作者信息

Urbani Simona, Amadei Barbara, Fisicaro Paola, Tola Daniela, Orlandini Alessandra, Sacchelli Luca, Mori Cristina, Missale Gabriele, Ferrari Carlo

机构信息

Laboratory of Viral Immunopathology, Department of Infectious Diseases and Hepatology, Azienda Ospedaliera di Parma, Parma, Italy.

出版信息

Hepatology. 2006 Jul;44(1):126-39. doi: 10.1002/hep.21242.

DOI:10.1002/hep.21242
PMID:16799989
Abstract

A timely, efficient, and coordinated activation of both CD4 and CD8 T cell subsets following HCV infection is believed to be essential for HCV control. However, to what extent a failure of the individual T cell subsets can contribute to the high propensity of HCV to persist is still largely undefined. To address this issue, we analyzed the breadth, vigor, and quality of CD4 and CD8 responses simultaneously with panels of peptides covering the entire HCV sequence or containing the HLA-A2-binding motif, and with recombinant HCV proteins in 16 patients with acute HCV infection by tetramer staining, ELISPOT, and intracellular cytokine staining for interferon gamma, interleukin (IL)-2, IL-4, and IL-10. Our results indicate that at clinical onset, CD8 responses are similarly weak and narrowly focused in both self-limited and chronically evolving infections. At this stage, CD4 responses are deeply impaired in patients with a chronic outcome as they are weak and of narrow specificity, unlike the strong, broad and T helper 1-oriented CD4 responses associated with resolving infections. Only patients able to finally control infection show maturation of CD8 memory sustained by progressive expansion of CD127+ CD8 cells. Thus, a poor CD8 response in the acute stage of infection may enhance the overall probability of chronic viral persistence. In conclusion, the presence of functional CD4 responses represents one of the factors dictating the fate of infection by directly contributing to control of the virus and by promoting maturation of protective memory CD8 responses.

摘要

丙肝病毒(HCV)感染后,CD4和CD8 T细胞亚群及时、高效且协调的激活被认为是控制HCV的关键。然而,单个T细胞亚群功能障碍在多大程度上导致HCV易于持续存在,目前仍不清楚。为解决这一问题,我们通过四聚体染色、ELISPOT以及针对干扰素γ、白细胞介素(IL)-2、IL-4和IL-10的细胞内细胞因子染色,使用覆盖整个HCV序列或包含HLA-A2结合基序的肽库以及重组HCV蛋白,同时分析了16例急性HCV感染患者的CD4和CD8反应的广度、强度和质量。我们的结果表明,在临床发病时,无论是自限性感染还是慢性进展性感染,CD8反应同样微弱且范围狭窄。在此阶段,慢性感染患者的CD4反应严重受损,表现为反应微弱且特异性狭窄,这与感染得到解决时出现的强烈、广泛且以辅助性T细胞1为主的CD4反应不同。只有最终能够控制感染的患者才会出现由CD127 + CD8细胞逐渐扩增维持的CD8记忆成熟。因此,感染急性期CD8反应不佳可能会增加慢性病毒持续存在的总体概率。总之,功能性CD4反应的存在是决定感染结局的因素之一,它通过直接控制病毒以及促进保护性记忆CD8反应的成熟来发挥作用。

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