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Sts-1的磷酸酶活性有助于抑制TCR信号传导。

A phosphatase activity of Sts-1 contributes to the suppression of TCR signaling.

作者信息

Mikhailik Anatoly, Ford Bradley, Keller James, Chen Yunting, Nassar Nicolas, Carpino Nick

机构信息

Department of Molecular Genetics and Microbiology, Room 130, Life Sciences Building, Stony Brook University, Stony Brook, NY 11794-5222, USA.

出版信息

Mol Cell. 2007 Aug 3;27(3):486-97. doi: 10.1016/j.molcel.2007.06.015.

DOI:10.1016/j.molcel.2007.06.015
PMID:17679096
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2709417/
Abstract

Precise signaling by the T cell receptor (TCR) is crucial for a proper immune response. To ensure that T cells respond appropriately to antigenic stimuli, TCR signaling pathways are subject to multiple levels of regulation. Sts-1 negatively regulates signaling pathways downstream of the TCR by an unknown mechanism(s). Here, we demonstrate that Sts-1 is a phosphatase that can target the tyrosine kinase Zap-70 among other proteins. The X-ray structure of the Sts-1 C terminus reveals that it has homology to members of the phosphoglycerate mutase/acid phosphatase (PGM/AcP) family of enzymes, with residues known to be important for PGM/AcP catalytic activity conserved in nature and position in Sts-1. Point mutations that impair Sts-1 phosphatase activity in vitro also impair the ability of Sts-1 to regulate TCR signaling in T cells. These observations reveal a PGM/AcP-like enzyme activity involved in the control of antigen receptor signaling.

摘要

T细胞受体(TCR)的精确信号传导对于适当的免疫反应至关重要。为确保T细胞对抗抗原刺激做出适当反应,TCR信号通路受到多层次的调控。Sts-1通过未知机制对TCR下游的信号通路进行负调控。在此,我们证明Sts-1是一种磷酸酶,除其他蛋白质外,它还能作用于酪氨酸激酶Zap-70。Sts-1 C末端的X射线结构显示,它与磷酸甘油酸变位酶/酸性磷酸酶(PGM/AcP)家族的酶具有同源性,已知对PGM/AcP催化活性重要的残基在Sts-1中按自然顺序和位置保守。在体外损害Sts-1磷酸酶活性的点突变也损害了Sts-1在T细胞中调节TCR信号传导的能力。这些观察结果揭示了一种参与控制抗原受体信号传导的PGM/AcP样酶活性。

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