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Seven-transmembrane receptor signalling and ERK compartmentalization.

机译:七跨膜受体信号传导和ERK分隔。

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摘要

Vast numbers of extracellular signalling molecules exert effects on their target cells by activation of a relatively limited number of mitogen-activated protein kinase (MAPK) cascades, raising the question of how specificity is achieved. To a large extent, this appears to be attributable to differences in kinetics and compartmentalization of MAPK protein activation that are dictated by MAPK-associated proteins serving as scaffolds, anchors, activators or effectors. Here, we review spatiotemporal aspects of signalling via the Ras-Raf-extracellular signal-regulated kinase pathway, emphasizing recent work on roles of arrestins as scaffolds and transducers for seven transmembrane receptor signalling.
机译:大量的细胞外信号分子通过激活相对有限数量的有丝分裂原激活的蛋白激酶(MAPK)级联反应,对其靶细胞产生作用,从而引发了如何实现特异性的问题。在很大程度上,这似乎归因于MAPK蛋白质激活的动力学和分区的差异,这是由充当支架,锚,激活物或效应子的MAPK相关蛋白质决定的。在这里,我们回顾了通过Ras-Raf-细胞外信号调节激酶途径进行信号传递的时空方面,强调了关于抑制蛋白作为7个跨膜受体信号转导的支架和换能器的最新研究。

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