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Literature DB >> 17679096

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

Anatoly Mikhailik¹, Bradley Ford, James Keller, Yunting Chen, Nicolas Nassar, Nick Carpino.

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.

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Year: 2007 PMID： 17679096 PMCID： PMC2709417 DOI： 10.1016/j.molcel.2007.06.015

Source DB: PubMed Journal: Mol Cell ISSN： 1097-2765 Impact factor: 17.970

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