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The complexities of G-protein-coupled receptor kinase function in Hedgehog signaling

机译:G蛋白偶联受体激酶功能在刺猬信号中的复杂性

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Hedgehog (Hh) signaling is essential for proper tissue patterning and maintenance and has a substantial impact on human disease. While many of the main components and mechanisms involved in transduction of the Hh signal have been identified, the details of how the pathway functions are continually being refined. One aspect that has attracted much attention recently is the involvement of G-protein-coupled receptor kinases (GRKs) in the pathway. These regulators of G-protein-coupled receptor (GPCR) signaling have an evolutionarily-conserved function in promoting high-threshold Hh target gene expression through regulation of Smoothened (Smo), a GPCR family member that activates intracellular Hh signaling. Several models of how GRKs impact on Smo to increase downstream signaling have been proposed. Recently, we demonstrated that these kinases have surprisingly complex and conflicting roles, acting to limit signaling through the pathway while also promoting Smo activity. In addition to the previously described direct effects of Gprk2 on Smo activation, Gprk2 also indirectly affects Hh signaling by controlling production of the second messenger cyclic AMP to influence protein kinase A activity.
机译:刺猬(Hh)信号对于正确的组织模式和维护至关重要,并且对人类疾病具有重大影响。虽然已经确定了涉及Hh信号转导的许多主要成分和机制,但有关途径功能的细节正在不断完善。最近引起广泛关注的一个方面是该途径中涉及G蛋白偶联受体激酶(GRK)。这些G蛋白偶联受体(GPCR)信号调节剂通过调节平滑化(Smo)(一种激活细胞内Hh信号传导的GPCR家族成员),在促进高阈值Hh靶基因表达方面具有进化上保守的功能。已经提出了几种关于GRK如何影响Smo以增加下游信号的模型。最近,我们证明了这些激酶具有令人惊讶的复杂和相互矛盾的作用,既可以限制该途径的信号传导,又可以促进Smo活性。除了先前描述的Gprk2对Smo激活的直接作用外,Gprk2还通过控制第二信使环AMP的产生来间接影响Hh信号传导,从而影响蛋白激酶A的活性。

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