热休克蛋白90通过限制异源二聚体的形成来抑制表皮生长因子受体2/人表皮生长因子受体2信号传导。
Hsp90 restrains ErbB-2/HER2 signalling by limiting heterodimer formation.
作者信息
Citri Ami, Gan Judith, Mosesson Yaron, Vereb Gyorgi, Szollosi Janos, Yarden Yosef
机构信息
Department of Biological Regulation, Weizmann Institute of Science, Rehovot 76100, Israel.
出版信息
EMBO Rep. 2004 Dec;5(12):1165-70. doi: 10.1038/sj.embor.7400300.
Abstract
ErbB-2/HER2 is an oncogenic tyrosine kinase that regulates a signalling network by forming ligand-induced heterodimers with several growth factor receptors of the ErbB family. Hsp90 and co-chaperones regulate degradation of ErbB-2 but not other ErbB members. Here, we report that the role of Hsp90 in modulating the ErbB network extends beyond regulation of protein stability. The capacity of ErbB-2 to recruit ligand-bound receptors into active heterodimers is limited by Hsp90, which is dissociated from ErbB-2 following ligand-induced heterodimerization. We show that Hsp90 binds a specific loop within the kinase domain of ErbB-2, thereby restraining heterodimer formation and catalytic function. These results define a role for Hsp90 as a molecular switch regulating the ErbB signalling network by limiting formation of ErbB-2-centred receptor complexes.
摘要
ErbB-2/HER2是一种致癌性酪氨酸激酶,它通过与ErbB家族的几种生长因子受体形成配体诱导的异二聚体来调节信号网络。热休克蛋白90(Hsp90)及其共伴侣蛋白调节ErbB-2的降解,但不调节其他ErbB家族成员。在此,我们报道Hsp90在调节ErbB网络中的作用超出了对蛋白质稳定性的调节。Hsp90限制了ErbB-2将配体结合的受体募集到活性异二聚体中的能力,在配体诱导的异二聚化后,Hsp90会从ErbB-2上解离。我们发现Hsp90结合ErbB-2激酶结构域内的一个特定环,从而抑制异二聚体形成和催化功能。这些结果确定了Hsp90作为分子开关的作用,通过限制以ErbB-2为中心的受体复合物的形成来调节ErbB信号网络。
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