首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Src homology domains in phospholipase C-gamma1 mediate its anti-apoptotic action through regulating the enzymatic activity.
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Src homology domains in phospholipase C-gamma1 mediate its anti-apoptotic action through regulating the enzymatic activity.

机译:磷脂酶C-gamma1中的Src同源结构域通过调节酶活性来介导其抗凋亡作用。

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摘要

Abstract Phospholipase-gamma1 (PLC-gamma1) prevents programmed cell death, for which the enzymatic activity has been implicated. However, the biological function of Src homology (SH) domains of PLC-gamma1 in promoting cell survival remains elusive. Here, we showed that deletion of the N-SH2 domain or both N-SH2 and C-SH2 domains, but not the SH3 domain, abolished the anti-apoptotic activity of PLC-gamma1. Surprisingly, removal of the whole SH domain inhibited apoptosis. The lipase-inactive PLC-gamma1 mutant (LIM) failed to suppress apoptosis. Moreover, the phospholipase activity in SH3- or whole SH domain-deleted cells was comparable to that of wild-type cells. By contrast, the enzymatic activity was substantially ablated in SH2 domain-deleted or LIM cells. A pharmacological inhibitor of PLC-gamma1 robustly diminished the anti-apoptotic action in wild-type, SH3- or whole SH domain-deleted cells, whereas pretreatment of SH2 domain-deleted or LIM cells with agents activating PKC and calcium mobilization markedly promoted cell survival. These results indicate that SH domains in PLC-gamma1 might mediate its anti-apoptotic action by regulating the enzymatic activity.
机译:摘要磷脂酶-γ1(PLC-gamma1)可以防止程序性细胞死亡,而这涉及酶的活性。但是,PLC-gamma1的Src同源(SH)域在促进细胞存活方面的生物学功能仍然难以捉摸。在这里,我们显示删除N-SH2域或N-SH2和C-SH2域,但不删除SH3域,消除了PLC-gamma1的抗凋亡活性。令人惊讶地,整个SH结构域的去除抑制了细胞凋亡。脂肪酶失活的PLC-gamma1突变体(LIM)无法抑制细胞凋亡。此外,SH3或整个SH结构域缺失的细胞中的磷脂酶活性与野生型细胞相当。相反,在SH2结构域缺失的或LIM细胞中,酶促活性基本上被消除。 PLC-gamma1的药理学抑制剂可强烈降低野生型,SH3或完整SH结构域缺失细胞中的抗凋亡作用,而用激活PKC和钙动员的试剂预处理SH2结构域缺失或LIM细胞则可显着促进细胞存活。这些结果表明,PLC-gamma1中的SH结构域可能通过调节酶活性来介导其抗凋亡作用。

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