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首页> 外文期刊>Current opinion in hematology >Recent advances on T-cell regulation by receptor tyrosine kinases.
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Recent advances on T-cell regulation by receptor tyrosine kinases.

机译:受体酪氨酸激酶对T细胞调节的最新进展。

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PURPOSE OF REVIEW: This review summarizes recent knowledge on the role of receptor tyrosine kinases, particularly erythropoietin-producing hepatocyte kinases (Ephs), in T-cell function and development. RECENT FINDINGS: Erythropoietin-producing hepatocyte kinase function and signaling in the immune system have been recently investigated. Cross-linking some Ephs results in T-cell costimulation and reduces the response threshold of T-cell receptor activation. In vivo, T-cell-mediated responses are compromised in EphB6 mice. Some Ephs are shown to control T-cell migration and adhesion, as well as the integrity of lymphoid organ structure. SUMMARY: Ephs are the largest family of receptor tyrosine kinases. Some Ephs are expressed in the lymphoid organs. Ephrins, ligands of Ephs, are also cell surface molecules. Cross-linking of certain Ephs facilitates T-cell activation and proliferation. Under physiologic conditions, such cross-linking by ephrins likely occurs in lymphoid organs, where ephrins on T cells interact with ephrins on the surface of neighboring fraternal T cells or antigen-presenting cells; this may explain why T-cell responses are more effectively initiated in the lymphoid organs. Certain Ephs are also critical for lymphocyte adhesion and migration and for proper lymphoid organ structure. Ephs and ephrins are highly redundant and their interactions promiscuous, suggesting pivotal roles of these molecules in biology. Conversely, such redundancy represents a major challenge to further dissection of the function of individual Ephs. Multiple tissue-specific gene null mutations on Ephs or ephrins will likely reveal more interesting immune-related phenotypes.
机译:综述的目的:这篇综述总结了有关受体酪氨酸激酶,特别是产生促红细胞生成素的肝细胞激酶(Ephs)在T细胞功能和发育中的作用的最新知识。最近的发现:最近研究了产生促红细胞生成素的肝细胞激酶功能和免疫系统中的信号传导。交联一些Eph会导致T细胞共刺激,并降低T细胞受体激活的反应阈值。在体内,T细胞介导的应答在EphB6小鼠中受损。一些Ephs被证明可以控制T细胞迁移和粘附以及淋巴器官结构的完整性。简介:Eph是受体酪氨酸激酶的最大家族。一些Ephs在淋巴器官中表达。 Ephrs的配体Ephrins也是细胞表面分子。某些Eph的交联促进T细胞活化和增殖。在生理条件下,ephrins的这种交联很可能发生在淋巴器官中,在T淋巴细胞上的ephrin与邻近的兄弟T细胞或抗原呈递细胞表面的ephrin相互作用。这可以解释为什么在淋巴器官中更有效地引发T细胞反应。某些Eph对于淋巴细胞粘附和迁移以及适当的淋巴器官结构也至关重要。 eph和ephrins是高度冗余的,它们之间的相互作用是混杂的,表明这些分子在生物学中起着关键作用。相反,这种冗余对进一步分离单个Eph的功能提出了重大挑战。 Ephs或ephrins上的多个组织特异性基因无效突变可能会揭示出更多有趣的免疫相关表型。

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