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丙型肝炎病毒暴露的健康血清阴性供体中效应性CD8 + T细胞的存在。

Presence of effector CD8+ T cells in hepatitis C virus-exposed healthy seronegative donors.

作者信息

Scognamiglio P, Accapezzato D, Casciaro M A, Cacciani A, Artini M, Bruno G, Chircu M L, Sidney J, Southwood S, Abrignani S, Sette A, Barnaba V

机构信息

Fondazione Andrea Cesalpino, Istituto di I Clinica Medica and Dipartimento di Malattie Infettive, Università di Roma La Sapienza, Italy.

出版信息

J Immunol. 1999 Jun 1;162(11):6681-9.

Abstract

CTL responses against multiple hepatitis C virus (HCV) epitopes were detected in 7 of 29 (24.1%) healthy family members (HFM) persistently exposed to chronically HCV-infected patients (HCV-HFM). These precursor CTL were at very low or undetectable frequencies, as determined by limiting dilution analysis. However, when HCV-specific effector CD8+ T cells, freshly isolated from PBMC of HCV-HFM, were assessed by a sensitive enzyme-linked immunospot assay, their frequencies were severalfold higher than those of precursor CTL. These results indicate that the two assays detect two functionally distinct T cell populations and that the effector cells are not assayed by the 51Cr-release assay. Furthermore, the combination of cell depletion and enzyme-linked immunospot analyses showed that the effector cells were confined into a CD8+ CD45RO+ CD28- population. The persistence of effector CD8+ T cells specific for both the structural and nonstructural viral proteins in uninfected HCV-HFM, suggest that: 1) an immunological memory is established upon a subclinical infection without any evidence of hepatitis, in a large cohort of HCV-exposed individuals; 2) because these cells required neither restimulation nor the addition of particular cytokines in vitro for differentiating in effectors, they should be capable of prompt HCV-specific effector function in vivo, possibly providing antiviral protection; and 3) the maintenance of effector T cell responses may be sustained by persisting low-level stimulation induced by inapparent infections.

摘要

在29名持续接触慢性丙型肝炎病毒感染患者(HCV-HFM)的健康家庭成员(HFM)中,有7名(24.1%)检测到针对多种丙型肝炎病毒(HCV)表位的CTL反应。通过有限稀释分析确定,这些前体CTL的频率非常低或无法检测到。然而,当通过灵敏的酶联免疫斑点试验评估从HCV-HFM的外周血单核细胞(PBMC)中新鲜分离的HCV特异性效应性CD8+T细胞时,其频率比前体CTL高几倍。这些结果表明,这两种检测方法检测到两种功能不同的T细胞群体,并且效应细胞不能通过51Cr释放试验进行检测。此外,细胞清除和酶联免疫斑点分析的结合表明,效应细胞局限于CD8+CD45RO+CD28-群体。未感染的HCV-HFM中针对病毒结构和非结构蛋白的效应性CD8+T细胞持续存在,这表明:1)在一大群接触HCV的个体中,在没有任何肝炎证据的亚临床感染后建立了免疫记忆;2)由于这些细胞在体外分化为效应细胞既不需要再刺激也不需要添加特定的细胞因子,它们应该能够在体内迅速发挥HCV特异性效应功能,可能提供抗病毒保护;3)效应性T细胞反应的维持可能由不明显感染诱导的持续低水平刺激所维持。

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