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粘着斑衔接蛋白PINCH LIM1结构域的溶液结构及其与整合素连接激酶锚蛋白重复结构域相互作用的表征

Solution structure of the focal adhesion adaptor PINCH LIM1 domain and characterization of its interaction with the integrin-linked kinase ankyrin repeat domain.

作者信息

Velyvis A, Yang Y, Wu C, Qin J

机构信息

Structural Biology Program, Lerner Research Institute, Cleveland Clinic Foundation, 9500 Euclid Ave., Cleveland, OH 44195, USA.

出版信息

J Biol Chem. 2001 Feb 16;276(7):4932-9. doi: 10.1074/jbc.M007632200. Epub 2000 Nov 14.

Abstract

PINCH is a recently identified adaptor protein that comprises an array of five LIM domains. PINCH functions through LIM-mediated protein-protein interactions that are involved in cell adhesion, growth, and differentiation. The LIM1 domain of PINCH interacts with integrin-linked kinase (ILK), thereby mediating focal adhesions via a specific integrin/ILK signaling pathway. We have solved the NMR structure of the PINCH LIM1 domain and characterized its binding to ILK. LIM1 contains two contiguous zinc fingers of the CCHC and CCCH types and adopts a global fold similar to that of functionally distinct LIM domains from cysteine-rich protein and cysteine-rich intestinal protein families with CCHC and CCCC zinc finger types. Gel-filtration and NMR experiments demonstrated a 1:1 complex between PINCH LIM1 and the ankyrin repeat domain of ILK. A chemical shift mapping experiment identified regions in PINCH LIM1 that are important for interaction with ILK. Comparison of surface features between PINCH LIM1 and other functionally different LIM domains indicated that the LIM motif might have a highly variable mode in recognizing various target proteins.

摘要

PINCH是一种最近被鉴定出的衔接蛋白,由五个LIM结构域组成。PINCH通过LIM介导的蛋白质-蛋白质相互作用发挥功能,这些相互作用涉及细胞黏附、生长和分化。PINCH的LIM1结构域与整合素连接激酶(ILK)相互作用,从而通过特定的整合素/ILK信号通路介导黏着斑。我们已经解析了PINCH LIM1结构域的核磁共振结构,并对其与ILK的结合进行了表征。LIM1包含两个相邻的CCHC型和CCCH型锌指,其整体折叠结构与富含半胱氨酸蛋白家族和富含半胱氨酸肠蛋白家族中功能不同的具有CCHC和CCCC锌指类型的LIM结构域相似。凝胶过滤和核磁共振实验证明PINCH LIM1与ILK的锚蛋白重复结构域之间形成了1:1复合物。化学位移映射实验确定了PINCH LIM1中对与ILK相互作用重要的区域。PINCH LIM1与其他功能不同的LIM结构域表面特征的比较表明,LIM基序在识别各种靶蛋白时可能具有高度可变的模式。

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