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Is there a place and role for endocytic TCR TCR signaling?

机译:是否存在对内吞TCR信号传导的地方和角色?

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Abstract T‐lymphocyte activation relies on the cognate recognition by the TCR of the MHC‐associated peptide ligand (pMHC) presented at the surface of an antigen‐presenting cell (APC). This leads to the dynamic formation of a cognate contact between the T lymphocyte and the APC: the immune synapse (IS). Engagement of the TCR by the pMHC in the synaptic zone induces a cascade of signaling events leading to phosphorylation and dephosphorylation of proteins and lipids, which ultimately shapes the response of T lymphocytes. Although the engagement of the T‐cell receptor (TCR) takes place at the plasma membrane, the TCR/CD3 complexes and the signaling molecules involved in transduction of the TCR signal are also present in intracellular membrane pools. These pools, which are both endocytic and exocytic, have tentatively been characterized by several groups including ours. We will herein summarize what is known on the intracellular pools of TCR signaling components. We will discuss their origin and the mechanisms involved in their mobility at the IS. Finally, we will propose several hypotheses concerning the functional role(s) that these intracellular pools might play in T‐cell activation. We will also discuss the tools that could be used to test these hypotheses.
机译:摘要T淋巴细胞激活依赖于在抗原呈递细胞(APC)表面上的MHC相关肽配体(PMHC)的TCR的同源识别。这导致T淋巴细胞和APC之间的同源接触的动态形成:免疫突触(是)。 TCR在突触区中的PMHC接合引起级联的信号传导事件,导致蛋白质和脂质的磷酸化和去磷酸化,这最终塑造了T淋巴细胞的响应。尽管T细胞受体(TCR)的接合发生在质膜上,但TCR / CD3络合物和参与TCR信号的转导的信号分子也存在于细胞内膜池中。这些池是内吞和卵细胞,暂时的特征在于包括我们的几组。我们将在本文中总结了在TCR信号传导组分的细胞内池中所知的内容。我们将讨论他们的起源和涉及他们在流动性的机制。最后,我们将提出有关这些细胞内池在T细胞活化中起作用的功能作用的几个假设。我们还将讨论可用于测试这些假设的工具。

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