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首页> 外文期刊>Molecular and Cellular Biology >Role of diacylglycerol-regulated protein kinase C isotypes in growth factor activation of the Raf-1 protein kinase.
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Role of diacylglycerol-regulated protein kinase C isotypes in growth factor activation of the Raf-1 protein kinase.

机译:二酰基甘油调节的蛋白激酶C同种型在Raf-1蛋白激酶的生长因子激活中的作用。

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The Raf protein kinases function downstream of Ras guanine nucleotide-binding proteins to transduce intracellular signals from growth factor receptors. Interaction with Ras recruits Raf to the plasma membrane, but the subsequent mechanism of Raf activation has not been established. Previous studies implicated hydrolysis of phosphatidylcholine (PC) in Raf activation; therefore, we investigated the role of the epsilon isotype of protein kinase C (PKC), which is stimulated by PC-derived diacylglycerol, as a Raf activator. A dominant negative mutant of PKC epsilon inhibited both proliferation of NIH 3T3 cells and activation of Raf in COS cells. Conversely, overexpression of active PKC epsilon stimulated Raf kinase activity in COS cells and overcame the inhibitory effects of dominant negative Ras in NIH 3T3 cells. PKC epsilon also stimulated Raf kinase in baculovirus-infected Spodoptera frugiperda Sf9 cells and was able to directly activate Raf in vitro. Consistent with its previously reported activity as a Raf activator in vitro, PKC alpha functioned similarly to PKC epsilon in both NIH 3T3 and COS cell assays. In addition, constitutively active mutants of both PKC alpha and PKC epsilon overcame the inhibitory effects of dominant negative mutants of the other PKC isotype, indicating that these diacylglycerol-regulated PKCs function as redundant activators of Raf-1 in vivo.
机译:Raf蛋白激酶在Ras鸟嘌呤核苷酸结合蛋白的下游起作用,以转导来自生长因子受体的细胞内信号。与Ras的相互作用将Raf募集至质膜,但尚未确定Raf激活的后续机制。先前的研究涉及磷脂酰胆碱(PC)在Raf活化中的水解。因此,我们研究了由PC衍生的二酰基甘油刺激的蛋白激酶C(PKC)ε同种型作为Raf激活剂的作用。 PKCε的显性负突变体同时抑制NIH 3T3细胞的增殖和COS细胞中Raf的激活。相反,活性PKCε的过表达刺激了COS细胞中的Raf激酶活性,并克服了NIH 3T3细胞中显性负性Ras的抑制作用。 PKC epsilon还可以刺激杆状病毒感染的草地贪夜蛾Sf9细胞中的Raf激酶,并且能够在体外直接激活Raf。与先前报道的在体外作为Raf激活剂的活性一致,在NIH 3T3和COS细胞分析中,PKCα的功能与PKC epsilon相似。此外,PKCα和PKC epsilon的组成型活性突变体克服了其他PKC同种型的显性负突变体的抑制作用,表明这些二酰基甘油调节的PKC在体内充当Raf-1的冗余激活剂。

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