Department of Oncology, Microbiology and Immunology, University of Fribourg, Fribourg, Switzerland.
Front Immunol. 2021 Feb 15;12:626019. doi: 10.3389/fimmu.2021.626019. eCollection 2021.
Tissue-resident CD8 T cells (CD8 T) populate lymphoid and non-lymphoid tissues after infections as first line of defense against re-emerging pathogens. To achieve host protection, CD8 T have developed surveillance strategies that combine dynamic interrogation of pMHC complexes on local stromal and hematopoietic cells with long-term residency. Factors mediating CD8 T residency include CD69, a surface receptor opposing the egress-promoting S1P1, CD49a, a collagen-binding integrin, and CD103, which binds E-cadherin on epithelial cells. Moreover, the topography of the tissues of residency may influence T retention and surveillance strategies. Here, we provide a brief summary of these factors to examine how CD8 T reconcile constant migratory behavior with their long-term commitment to local microenvironments, with a focus on epithelial barrier organs and exocrine glands with mixed connective-epithelial tissue composition.
组织驻留 CD8 T 细胞(CD8 T)在感染后会分布在淋巴和非淋巴组织中,作为抵御再次出现的病原体的第一道防线。为了实现宿主保护,CD8 T 已经开发出了监视策略,将对局部基质和造血细胞上 pMHC 复合物的动态询问与长期驻留相结合。介导 CD8 T 驻留的因素包括 CD69,一种与促进外渗的 S1P1 相反的表面受体、CD49a,一种胶原结合整合素,以及 CD103,它与上皮细胞上的 E-钙粘蛋白结合。此外,驻留组织的拓扑结构可能会影响 T 细胞的保留和监视策略。在这里,我们简要总结了这些因素,以研究 CD8 T 如何在其长期承诺于局部微环境的同时协调不断的迁移行为,重点关注上皮屏障器官和具有混合结缔组织-上皮组织组成的外分泌腺。
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