首页> 美国卫生研究院文献>Aging (Albany NY) >Heterotrimeric G proteins as emerging targets for network based therapy in cancer: End of a long futile campaign striking heads of a Hydra
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Heterotrimeric G proteins as emerging targets for network based therapy in cancer: End of a long futile campaign striking heads of a Hydra

机译:异三聚体G蛋白作为基于网络的癌症治疗的新兴靶标:一次漫长而徒劳的运动结束了九头蛇的袭击

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摘要

Most common diseases, e.g., cancer are driven by not one, but multiple cell surface receptors that trigger and sustain a pathologic signaling network. The largest fraction of therapeutic agents that target individual receptors/pathways eventually fail due to the emergence of compensatory mechanisms that reestablish the pathologic network. Recently, a rapidly emerging paradigm has revealed GIV/Girdin as a central platform for receptor cross-talk which integrates signals downstream of a myriad of cell surface receptors, and modulates several key pathways within downstream signaling network, all via non-canonical activation of trimeric G proteins. Unlike canonical signal transduction via G proteins, which is spatially and temporally restricted, the temporal and spatial features of non-canonical activation of G protein via GIV is unusually unrestricted. Consequently, the GIV●G protein interface serves as a central hub allowing for control over several pathways within the pathologic signaling network, all at once. The relevance of this new paradigm in cancer and other disease states and the pros and cons of targeting the GIV●G protein interface are discussed.
机译:最常见的疾病,例如癌症,不是由一种而是由多种细胞表面受体驱动的,这些细胞表面受体触发并维持病理信号网络。靶向个体受体/途径的最大部分治疗剂最终由于重建病理网络的补偿机制的出现而失败。最近,一种迅速兴起的范例揭示了GIV / Girdin作为受体串扰的中心平台,该平台整合了无数细胞表面受体下游的信号,并通过三聚体的非规范激活来调节下游信号网络内的几个关键途径。 G蛋白。与在空间和时间上受到限制的经由G蛋白的经典信号转导不同,经由GIV进行G蛋白的非经典激活的时空特征通常不受限制。因此,GIV·G蛋白接口可作为中央枢纽,从而一次即可控制病理信号网络中的多个途径。讨论了这种新范式在癌症和其他疾病状态中的相关性以及靶向GIV●G蛋白界面的利弊。

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