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内在无序在协调 Wnt 通路中的作用。

The roles of intrinsic disorder in orchestrating the Wnt-pathway.

机构信息

Department of Molecular Medicine, University of South Florida, Tampa, FL 33612, USA.

出版信息

J Biomol Struct Dyn. 2012;29(5):843-61. doi: 10.1080/073911012010525024.

Abstract

The canonical Wnt-pathway plays a number of crucial roles in the development of organism. Malfunctions of this pathway lead to various diseases including cancer. In the inactivated state, this pathway involves five proteins, Axin, CKI-α, GSK-3β, APC, and β-catenin. We analyzed these proteins by a number of computational tools, such as PONDR(r)VLXT, PONDR(r)VSL2, MoRF-II predictor and Hydrophobic Cluster Analysis (HCA) to show that each of the Wnt-pathway proteins contains several intrinsically disordered regions. Based on a comprehensive analysis of published data we conclude that these disordered regions facilitate protein-protein interactions, post-translational modifications, and signaling. The scaffold protein Axin and another large protein, APC, act as flexible concentrators in gathering together all other proteins involved in the Wnt-pathway, emphasizing the role of intrinsically disordered regions in orchestrating the complex protein-protein interactions. We further explore the intricate roles of highly disordered APC in regulation of β-catenin function. Intrinsically disordered APC helps the collection of β-catenin from cytoplasm, facilitates the b-catenin delivery to the binding sites on Axin, and controls the final detachment of β-catenin from Axin.

摘要

经典 Wnt 通路在生物体的发育中发挥着许多关键作用。该通路的功能障碍会导致各种疾病,包括癌症。在失活状态下,该通路涉及五种蛋白质:Axin、CKI-α、GSK-3β、APC 和 β-catenin。我们使用了许多计算工具对这些蛋白质进行了分析,如 PONDR(r)VLXT、PONDR(r)VSL2、MoRF-II 预测器和疏水区分析(HCA),结果表明每个 Wnt 通路蛋白都包含几个固有无序区域。基于对已发表数据的综合分析,我们得出结论,这些无序区域促进了蛋白质-蛋白质相互作用、翻译后修饰和信号转导。支架蛋白 Axin 和另一个大蛋白 APC 作为灵活的聚集器,聚集了所有参与 Wnt 通路的其他蛋白质,强调了固有无序区域在协调复杂的蛋白质-蛋白质相互作用中的作用。我们进一步探讨了高度无序的 APC 在调节 β-catenin 功能中的复杂作用。固有无序的 APC 有助于从细胞质中收集 β-catenin,促进 β-catenin 递送到 Axin 上的结合位点,并控制 β-catenin 与 Axin 的最终分离。

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