Veillette A, Horak I D, Horak E M, Bookman M A, Bolen J B
Laboratory of Tumor Virus Biology, National Cancer Institute, Bethesda, Maryland 20892.
Mol Cell Biol. 1988 Oct;8(10):4353-61. doi: 10.1128/mcb.8.10.4353-4361.1988.
The lymphocyte-specific tyrosine protein kinase p56lck is abundantly expressed in L3T4+ (CD4+) and Lyt-2+ (CD8+) T-lymphocytes, where it is predominantly phosphorylated in vivo on the carboxy-terminal tyrosine residue 505 (Y-505). Upon exposure to activating signals (mitogenic lectins, antibodies to the T-cell receptor), the p56lck expressed in normal cloned murine T-cells is modified into a product which migrates at approximately 59 kilodaltons on sodium dodecyl sulfate-polyacrylamide gels and which possesses several amino-terminal serine phosphorylations. The changes in both mobility and amino-terminal phosphorylation can be reproduced by known activators of protein kinase C (4 alpha-phorbol 12 beta-myristate, dioctanoylglycerol), suggesting that this signal transduction pathway (or related pathways) mediates at least part of these events. Interestingly, agents raising intracellular calcium (such as A23187) cause the appearance of several of these amino-terminal phosphorylation changes but do not cause the pronounced shift in electrophoretic mobility. These data suggest that at least two serine kinase systems are implicated in the alterations of p56lck associated with T-cell activation and that the lck gene product plays a critical role in normal T-cell physiology.
淋巴细胞特异性酪氨酸蛋白激酶p56lck在L3T4 +(CD4 +)和Lyt-2 +(CD8 +)T淋巴细胞中大量表达,在体内它主要在羧基末端酪氨酸残基505(Y - 505)处被磷酸化。在暴露于激活信号(促有丝分裂凝集素、抗T细胞受体抗体)后,正常克隆的鼠T细胞中表达的p56lck被修饰为一种产物,该产物在十二烷基硫酸钠 - 聚丙烯酰胺凝胶上以约59千道尔顿的分子量迁移,并且具有几个氨基末端丝氨酸磷酸化。迁移率和氨基末端磷酸化的变化可以由蛋白激酶C的已知激活剂(4α - 佛波醇12β - 肉豆蔻酸酯、二辛酰甘油)重现,这表明该信号转导途径(或相关途径)介导了这些事件的至少一部分。有趣的是,提高细胞内钙的试剂(如A23187)会导致其中一些氨基末端磷酸化变化的出现,但不会导致电泳迁移率的明显改变。这些数据表明,至少有两个丝氨酸激酶系统与T细胞激活相关的p56lck改变有关,并且lck基因产物在正常T细胞生理学中起关键作用。
