Regulation of T Cell Receptor Signaling by Tyrosine Phosphatase SYP Association with CTLA-4

Luc E. M. Marengère; Paul Waterhouse; Gordon S. Duncan; Hans‐Willi Mittrücker; Gen‐Sheng Feng; Tak W. Mak

doi:10.1126/science.272.5265.1170

Regulation of T Cell Receptor Signaling by Tyrosine Phosphatase SYP Association with CTLA-4

Luc E. M. Marengère(Ontario Institute for Cancer Research), Paul Waterhouse(Ontario Institute for Cancer Research), Gordon S. Duncan(Ontario Institute for Cancer Research), Hans‐Willi Mittrücker(Ontario Institute for Cancer Research), Gen‐Sheng Feng(Walther Cancer Foundation), Tak W. Mak(Ontario Institute for Cancer Research)

Science

May 24, 1996

10.1126/science.272.5265.1170

Cited by 568

Abstract

The absence of CTLA-4 results in uncontrolled T cell proliferation. The T cell receptor-specific kinases FYN, LCK, and ZAP-70 as well as the RAS pathway were found to be activated in T cells of Ctla-4-/- mutant mice. In addition, CTLA-4 specifically associated with the tyrosine phosphatase SYP, an interaction mediated by the SRC homology 2 (SH2) domains of SYP and the phosphotyrosine sequence Tyr-Val-Lys-Met within the CTLA-4 cytoplasmic tail. The CTLA-4-associated SYP had phosphatase activity toward the RAS regulator p52SHC. Thus, the RAS pathway and T cell activation through the T cell receptor are regulated by CTLA-4-associated SYP.

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