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SLP-76 N端酪氨酸的功能层级

Functional hierarchy of the N-terminal tyrosines of SLP-76.

作者信息

Jordan Martha S, Sadler Jeffrey, Austin Jessica E, Finkelstein Lisa D, Singer Andrew L, Schwartzberg Pamela L, Koretzky Gary A

机构信息

Signal Transduction Program, Leonard and Madlyn Abramson Family Cancer Research Institute, University of Pennsylvania School of Medicine, Philadelphia, 19104, USA.

出版信息

J Immunol. 2006 Feb 15;176(4):2430-8. doi: 10.4049/jimmunol.176.4.2430.

Abstract

The adaptor protein Src homology 2 domain-containing leukocyte phosphoprotein of 76 kDa (SLP-76) plays a central role in T cell activation and T cell development. SLP-76 has three functional modules: an acidic domain with three key tyrosines, a central proline-rich domain, and a C-terminal Src homology 2 domain. Of these, mutation of the three N-terminal tyrosines (Y112, Y128, and Y145) results in the most profound effects on T cell development and function. Y112 and Y128 associate with Vav and Nck, two proteins shown to be important for TCR-induced phosphorylation of proximal signaling substrates, Ca(2+) flux, and actin reorganization. Y145 has been shown to be important for optimal association of SLP-76 with inducible tyrosine kinase, a key regulator of T cell function. To investigate further the role of the phosphorylatable tyrosines of SLP-76 in TCR signaling, cell lines and primary T cells expressing SLP-76 with mutations in individual or paired tyrosine residues were analyzed. These studies show that Tyr(145) of SLP-76 is the most critical tyrosine for both T cell function in vitro and T cell development in vivo.

摘要

衔接蛋白含Src同源2结构域的76 kDa白细胞磷蛋白(SLP-76)在T细胞活化和T细胞发育中起核心作用。SLP-76有三个功能模块:一个带有三个关键酪氨酸的酸性结构域、一个富含脯氨酸的中央结构域和一个C端Src同源2结构域。其中,三个N端酪氨酸(Y112、Y128和Y145)的突变对T细胞发育和功能产生最深远的影响。Y112和Y128与Vav和Nck结合,这两种蛋白对TCR诱导的近端信号底物磷酸化、Ca(2+)通量和肌动蛋白重组很重要。Y145已被证明对SLP-76与诱导型酪氨酸激酶(T细胞功能的关键调节因子)的最佳结合很重要。为了进一步研究SLP-76的可磷酸化酪氨酸在TCR信号传导中的作用,分析了表达单个或成对酪氨酸残基突变的SLP-76的细胞系和原代T细胞。这些研究表明,SLP-76的Tyr(145)对于体外T细胞功能和体内T细胞发育都是最关键的酪氨酸。

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