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一个大规模的亨廷顿蛋白相互作用网络提示亨廷顿病中的 Rho GTP 酶信号通路。

A large scale Huntingtin protein interaction network implicates Rho GTPase signaling pathways in Huntington disease.

机构信息

Buck Institute for Research on Aging, Novato, California 94945.

Prolexys Pharmaceuticals, Salt Lake City, Utah 84116; Huntsman Cancer Institute, University of Utah, Salt Lake City, Utah 84112.

出版信息

J Biol Chem. 2014 Mar 7;289(10):6709-6726. doi: 10.1074/jbc.M113.523696. Epub 2014 Jan 9.

Abstract

Huntington disease (HD) is an inherited neurodegenerative disease caused by a CAG expansion in the HTT gene. Using yeast two-hybrid methods, we identified a large set of proteins that interact with huntingtin (HTT)-interacting proteins. This network, composed of HTT-interacting proteins (HIPs) and proteins interacting with these primary nodes, contains 3235 interactions among 2141 highly interconnected proteins. Analysis of functional annotations of these proteins indicates that primary and secondary HIPs are enriched in pathways implicated in HD, including mammalian target of rapamycin, Rho GTPase signaling, and oxidative stress response. To validate roles for HIPs in mutant HTT toxicity, we show that the Rho GTPase signaling components, BAIAP2, EZR, PIK3R1, PAK2, and RAC1, are modifiers of mutant HTT toxicity. We also demonstrate that Htt co-localizes with BAIAP2 in filopodia and that mutant HTT interferes with filopodial dynamics. These data indicate that HTT is involved directly in membrane dynamics, cell attachment, and motility. Furthermore, they implicate dysregulation in these pathways as pathological mechanisms in HD.

摘要

亨廷顿病(HD)是一种由 HTT 基因中的 CAG 扩展引起的遗传性神经退行性疾病。我们使用酵母双杂交方法鉴定了一大组与亨廷顿蛋白(HTT)相互作用的蛋白质。该网络由 HTT 相互作用蛋白(HIPs)和与这些主要节点相互作用的蛋白质组成,包含 3235 个相互作用,涉及 2141 个高度相互连接的蛋白质。对这些蛋白质的功能注释分析表明,主要和次要 HIPs 富含与 HD 相关的途径,包括雷帕霉素靶蛋白、Rho GTPase 信号和氧化应激反应。为了验证 HIPs 在突变 HTT 毒性中的作用,我们表明 Rho GTPase 信号成分 BAIAP2、EZR、PIK3R1、PAK2 和 RAC1 是突变 HTT 毒性的调节剂。我们还证明 Htt 与 BAIAP2 在丝状伪足中共定位,并且突变 HTT 干扰丝状伪足的动力学。这些数据表明 HTT 直接参与膜动力学、细胞附着和运动。此外,它们表明这些途径的失调是 HD 的病理机制。

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