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T Cell Receptor ap Diversity Inversely Correlates with Pathogen-Specific Antibody Levels in Human Cytomegalovirus Infection

机译:T细胞受体ap多样性与人类巨细胞病毒感染的病原体特异性抗体水平成反比。

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A diverse T cell receptor (TCR) repertoire capable of recognizing a broad range of antigenic peptides is thought to be central to effective pathogen-specific immunity by counteracting escape mutations, selecting high-avidity T cells, and providing T cell specificities with comprehensive functional characteristics. However, evidence that TCR diversity is important for the successful control of human infections is limited. A single-cell strategy for the clonotypic analysis of human CD8+ TCRaP repertoires was used to probe the diversity and magnitude of individual human cytomegalovirus (CMV)-specific CD8+ T cells recovered directly ex vivo. We found that CD8+ TCRaP repertoire diversity, but not the size of the CD8+ T cell response, was inversely related to circulating CMV-specific antibody levels, a measure that has been correlated epidemiologically with differential mortality risks and found here to be higher in persons with detectable (versus undetectable) CMV viral loads. Overall, our findings indicate that CD8+ T cell diversity may be more important than T cell abundance in limiting the negative consequences of CMV persistence, demonstrate high prevalence of both TCRa and TCRp public motif usage, and suggest that a highly diverse TCRaP repertoire may be an important benchmark and target in the success of immunotherapeutic strategies.
机译:可以识别多种抗原肽的多样化T细胞受体(TCR)库被认为是有效的病原体特异性免疫的关键,它可以抵消逃逸突变,选择高存活率T细胞并提供具有全面功能特征的T细胞特异性。但是,TCR多样性对于成功控制人类感染至关重要的证据有限。使用单细胞策略对人CD8 + TCRaP曲目进行克隆型分析,以探查直接从离体体内回收的单个人巨细胞病毒(CMV)特异性CD8 + T细胞的多样性和大小。我们发现,CD8 + TCRaP的库多样性与CD8 + T细胞反应的大小无关,与循环CMV特异性抗体水平成反比,该方法已在流行病学上与不同的死亡风险相关,并且在患有以下疾病的人中较高可检测(相对于不可检测)的CMV病毒载量。总体而言,我们的发现表明,在限制CMV持久性的负面后果方面,CD8 + T细胞的多样性可能比T细胞的丰富度更重要,证明TCRa和TCRp公共基序用法的普遍性很高,并表明高度多样性的TCRaP曲目可能是是免疫治疗策略成功的重要基准和目标。

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