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Clonal selection in the human Vδ1 T cell repertoire indicates γδ TCR-dependent adaptive immune surveillance

机译:人类Vδ1T细胞库中的克隆选择表明γδTCR依赖的自适应免疫监视

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摘要

γδ T cells are considered to be innate-like lymphocytes that respond rapidly to stress without clonal selection and differentiation. Here we use next-generation sequencing to probe how this paradigm relates to human Vδ2neg T cells, implicated in responses to viral infection and cancer. The prevalent Vδ1 T cell receptor (TCR) repertoire is private and initially unfocused in cord blood, typically becoming strongly focused on a few high-frequency clonotypes by adulthood. Clonal expansions have differentiated from a naive to effector phenotype associated with CD27 downregulation, retaining proliferative capacity and TCR sensitivity, displaying increased cytotoxic markers and altered homing capabilities, and remaining relatively stable over time. Contrastingly, Vδ2+ T cells express semi-invariant TCRs, which are present at birth and shared between individuals. Human Vδ1+ T cells have therefore evolved a distinct biology from the Vδ2+ subset, involving a central, personalized role for the γδ TCR in directing a highly adaptive yet unconventional form of immune surveillance.
机译:γδT细胞被认为是先天性淋巴细胞,可对应激快速反应,而无需克隆选择和分化。在这里,我们使用下一代测序技术来探究这种范例与人类Vδ2 neg T细胞之间的关系,并涉及对病毒感染和癌症的反应。常见的Vδ1T细胞受体(TCR)曲目是私人的,最初不集中在脐带血中,通常到成年后便会强烈地集中在一些高频克隆型上。克隆扩增已从与CD27下调相关的幼稚表型转变为效应子表型,保留了增殖能力和TCR敏感性,显示出增加的细胞毒性标记物和改变的归巢能力,并且随着时间的推移保持相对稳定。相反,Vδ2 + T细胞表达半不变的TCR,这些TCR在出生时就存在并在个体之间共享。因此,人类Vδ1 + T细胞已从Vδ2 + 子集发展出独特的生物学特性,涉及γδTCR在指导高度适应性但非常规形式的γδTCR中的核心个性化作用。免疫监视。

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