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首页> 外文期刊>The Journal of Experomental Medicine >Antigen-dependent competition shapes the local repertoire of tissue-resident memory CD8+ T cells
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Antigen-dependent competition shapes the local repertoire of tissue-resident memory CD8+ T cells

机译:抗原依赖性竞争决定了组织驻留记忆CD8 + T细胞的局部组成

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Tissue-resident memory CD8+ T cells (TRM) constitute a major component of the immune-surveillance system in nonlymphoid organs. Local, noncognate factors are both necessary and sufficient to support the programming of TRM cell fate in tissue-infiltrating T cells. Recent evidence suggests that TCR signals received in infected nonlymphoid tissues additionally contribute to TRM cell formation. Here, we asked how antigen-dependent pathways influence the generation of skin-resident memory T cells that arise from a polyclonal repertoire of cells induced by infection with an antigenically complex virus and recombinant vaccine vector. We found that CD8+ T cells of different specificities underwent antigen-dependent competition in the infected tissue, which shaped the composition of the local pool of TRM cells. This local cross-competition was active for T cells recognizing antigens that are coexpressed by infected cells. In contrast, TRM cell development remained largely undisturbed by the presence of potential competitors when antigens expressed in the same tissue were segregated through infection with antigenically distinct viral quasispecies. Functionally, local cross-competition might serve as a gatekeeping mechanism to regulate access to the resident memory niche and to fine-tune the local repertoire of antiviral TRM cells.
机译:组织驻留记忆CD8 + T细胞(TRM)构成非淋巴器官免疫监视系统的主要组成部分。局部非同源因子既必要又足以支持组织浸润T细胞中TRM细胞命运的编程。最近的证据表明,感染的非淋巴组织中收到的TCR信号还有助于TRM细胞的形成。在这里,我们问抗原依赖性途径如何影响皮肤驻留性记忆T细胞的产生,这种记忆性T细胞是由抗原复合病毒和重组疫苗载体感染诱导的细胞多克隆库所产生的。我们发现不同特异性的CD8 + T细胞在受感染的组织中经历了抗原依赖性竞争,从而形成了TRM细胞局部池的组成。这种局部交叉竞争对识别被感染细胞共表达的抗原的T细胞具有活性。相反,当在同一组织中表达的抗原通过感染抗原性不同的病毒准种而分离时,TRM细胞的发育在很大程度上不受潜在竞争者的干扰。从功能上讲,局部交叉竞争可以作为一种守门机制,以调节对常驻记忆位的访问,并微调抗病毒TRM细胞的局部组成。

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