STRUCTURAL REQUIREMENTS FOR ENHANCEMENT OF T-CELL RESPONSIVENESS BY THE LYMPHOCYTE-SPECIFIC TYROSINE PROTEIN-KINASE P56LCK

被引:99
|
作者
CARON, L
ABRAHAM, N
PAWSON, T
VEILLETTE, A
机构
[1] MCGILL UNIV, MCGILL CANC CTR, MONTREAL H3A 2T5, QUEBEC, CANADA
[2] MCGILL UNIV, DEPT MED, MONTREAL H3A 2T5, QUEBEC, CANADA
[3] MCGILL UNIV, DEPT BIOCHEM, MONTREAL H3A 2T5, QUEBEC, CANADA
[4] MCGILL UNIV, DEPT ONCOL, MONTREAL H3A 2T5, QUEBEC, CANADA
[5] MONTREAL GEN HOSP, DEPT MED, DIV MED ONCOL, MONTREAL H3G 1A4, QUEBEC, CANADA
[6] MT SINAI HOSP, SAMUEL LUNENFELD RES INST, TORONTO M5G 1X5, ONTARIO, CANADA
来源
MOLECULAR AND CELLULAR BIOLOGY | 1992年 / 12卷 / 06期
关键词
D O I
10.1128/MCB.12.6.2720
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
To understand the mechanism(s) by which p56lck participates in T-cell receptor (TCR) signalling, we have examined the effects of mutations in known regulatory domains of p56lck on the ability of F505 p56lck to enhance the responsiveness of an antigen-specific murine T-cell hybridoma. A mutation of the amino-terminal site of myristylation (glycine 2), which prevents stable association of p56lck with the plasma membrane, completely abolished the ability of F505 p56lck to enhance TCR-induced tyrosine protein phosphorylation. Alteration of the major site of in vitro autophosphorylation, tyrosine 394, to phenylalanine diminished the enhancement of TCR-induced tyrosine protein phosphorylation by F505 p56lck. Such a finding is consistent with the previous demonstration that this site is required for full activation of p56lck by mutation of tyrosine 505. Strikingly, deletion of the noncatalytic Src homology domain 2, but not of the Src homology domain 3, markedly reduced the improvement of TCR-induced tyrosine protein phosphorylation by F505 Lck. Additional studies revealed that all the mutations tested, including deletion of the Src homology 3 region, abrogated the enhancement of antigen-triggered interleukin-2 production by F505 p56lck, thus implying more stringent requirements for augmentation of antigen responsiveness by F505 Lck. Finally, it was also observed that expression of F505 p56lck greatly increased TCR-induced tyrosine phosphorylation of phospholipase C-gamma(1), raising the possibility that phospholipase C-gamma(1) may be a substrate for p56lck in T lymphocytes. Our results indicate that p56lck regulates T-cell antigen receptor signalling through a complex process requiring multiple distinct structural domains of the protein.
引用
收藏
页码:2720 / 2729
页数:10
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