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Solution structure and biophysical characterization of the multifaceted signalling effector protein growth arrest specific-1

机译:溶液结构和生物物理表征的多面信号效应蛋白生长阻滞特异性1

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摘要

BackgroundThe protein growth arrest specific-1 (GAS1) was discovered based on its ability to stop the cell cycle. During development it is involved in embryonic patterning, inhibits cell proliferation and mediates cell death, and has therefore been considered as a tumor suppressor. GAS1 is known to signal through two different cell membrane receptors: Rearranged during transformation (RET), and the sonic hedgehog receptor Patched-1. Sonic Hedgehog signalling is important in stem cell renewal and RET mediated signalling in neuronal survival. Disorders in both sonic hedgehog and RET signalling are connected to cancer progression. The neuroprotective effect of RET is controlled by glial cell-derived neurotrophic factor family ligands and glial cell-derived neurotrophic factor receptor alphas (GFRαs). Human Growth arrest specific-1 is a distant homolog of the GFRαs.
机译:背景蛋白质生长停滞特异性-1(GAS1)是基于其停止细胞周期的能力而发现的。在发育过程中,它参与胚胎构图,抑制细胞增殖并介导细胞死亡,因此被认为是肿瘤抑制剂。已知GAS1通过两种不同的细胞膜受体发出信号:转化过程中的重排(RET)和声波刺猬受体Patched-1。声波刺猬信号在干细胞更新和RET介导的神经元存活中起重要作用。声波刺猬和RET信号障碍均与癌症进展有关。 RET的神经保护作用受神经胶质细胞源性神经营养因子家族配体和神经胶质细胞源性神经营养因子受体α(GFRαs)的控制。人类生长停滞特异性1是GFRα的遥远同源物。

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