PHOSPHORYLATION OF SERINE-59 OF P56(LCK) IN ACTIVATED T-CELLS

被引：0

作者：

WATTS, JD

SANGHERA, JS

PELECH, SL

AEBERSOLD, R

机构：

[1] UNIV BRITISH COLUMBIA, BIOMED RES CTR, 2222 HLTH SCI MALL, VANCOUVER V6T 1Z3, BC, CANADA

[2] UNIV BRITISH COLUMBIA, DEPT BIOCHEM, VANCOUVER V6T 1W5, BC, CANADA

[3] UNIV BRITISH COLUMBIA, DEPT MED, VANCOUVER V6T 1W5, BC, CANADA

[4] KINETEK BIOTECHNOL CORP, RICHMOND V7C 1T6, BC, CANADA

来源：

JOURNAL OF BIOLOGICAL CHEMISTRY | 1993年 / 268卷 / 31期

关键词：

D O I：

暂无

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

p56lck, a member of the src family of non-receptor protein tyrosine kinases, is expressed almost exclusively in cells of lymphoid origin. Recent evidence has implicated p56lck in a critical role both in T cell development and activation. A variety of T cell stimuli induce a shift in the electrophoretic mobility of p56lck from an apparent molecular mass of 56 kDa (p56lck) to 60 kDa (p60lck). This shift in electrophoretic mobility correlates with an increase in the phosphoserine content of the p60lck. We have shown that both 4alpha-phorbol 12beta-myristate acetate and OKT3 treatment of Jurkat cells, as well as 4alpha-phorbol 12beta-myristate acetate treatment of 171.CD4 and LSTRA cells, induced phosphorylation of serine-59 on p56lck in vivo, which correlated with the shift to p60lck. We also demonstrated that the same serine residue could be phosphorylated in vitro with mitogen-activated protein kinases and that this event was capable of reducing p56lck activity in vitro. Combined, these data suggest a novel pathway for the in vivo regulation of p56lck activity.

引用

页码：23275 / 23282

页数：8

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