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The CNS Immune Landscape from the Viewpoint of a T Cell

机译:从T细胞的角度来看,CNS免疫景观

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Neuro-immune interactions are not only vital for the control of neurotropic pathogens, but also appear to influence brain development and homeostasis. During immune surveillance, T cells can patrol the CNS-associated border regions to sense pathogenic alterations. While access to the CNS parenchyma is restricted in the steady state, various disease processes can initiate parenchymal T cell CNS invasion. However, to breach the glia limitans, T cellsmust become reactivated within the meningeal spaces. T cells cannot sense native antigens (Ags), but instead recognize small processed peptides bound to MHC molecules and presented on the surface of Ag-presenting cells (APCs). In this review, we focus on (CD4(+)) T cell-CNS interactions that are dependent on Ag recognition. We discuss the potential paths and mechanisms of T cell entry into the CNS, in particular with respect to CNS-resident APCs, which present CNS-derived Ag in the absence of inflammation.
机译:神经免疫相互作用不仅对控制神经疗促病原体至关重要,而且似乎影响大脑发育和稳态。 在免疫监测期间,T细胞可以巡逻CNS相关的边境区域以感知病原改变。 虽然在稳定状态下限制了CNS薄壁症的进入,但各种疾病方法可以引发实质T细胞CNS侵袭。 然而,为了违反Glia巨大体,T细胞在脑膜空间内重新激活。 T细胞不能感知天然抗原(AGS),而是识别与MHC分子结合的小加工肽并呈现在Ag呈递细胞(APC)的表面上。 在此述评中,我们专注于(CD4(+))T Cell-CNS交互,这些交互取决于AG识别。 我们讨论T细胞进入CNS的潜在路径和机制,特别是关于CNS族APC,其在没有炎症的情况下存在CNS衍生的AG。

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