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Rap1, a Ras-like GTPase with a Distinct Function

机译:RAP1,RAS样GTP酶,功能明显

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摘要

Rapl is a very close relative of Ras, but its function is likely to be distinct. A novel assay was developed to measure activation of Rapl and it was found that a large variety of extracellular stimuli are able to activate this small GTPase very rapidly. Common second messengers, like calcium, diacylglycerol and cAMP mediate this activation in a cell type dependent manner. We have studied the molecular mechanism of these activations and one of the striking results was the discovery of Epac, a novel binding protein of cAMP. Epac is a guanine nucleotide exchange protein for Rapl. This finding indicates that the common notion that all effects of cAMP are mediated by protein kinase A is incorrect. The function of Rapl is largely unknown. Recent evidence indicates that the hypothesis that Rapl functions as an antagonist of Ras effector signalling is probably incorrect. More like Rapl mediates a distinct pathway regulating processes related to the control of the actin cytoskeleton affecting vesicular traficking and/or cell adhesion.
机译:Rapl是RAS非常紧密的,但其功能可能是截然不同的。开发了一种新的测定来测量Rapl的激活,发现各种细胞外刺激能够非常快速地激活这种小GTP酶。常见的第二次信使,如钙,二酰基甘油和阵营以细胞类型依赖性方式介导这种激活。我们研究了这些激活的分子机制,其中一个引人注目的结果是EPAC的发现,这是营地的一种新型结合蛋白。 EPAC是鸟嘌呤核苷酸交换蛋白,用于RAPL。这一发现表明,阵营的所有效果都是蛋白激酶A介导的常见观念是不正确的。 Rapl的功能在很大程度上是未知的。最近的证据表明,Rapl作为RAS效应信号传导的拮抗剂的假设可能不正确。更像Rapl介导与影响肌蛋白细胞骨架的控制有关的不同的途径调节过程,影响囊泡特征和/或细胞粘附。

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