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涉及多模块蛋白的机械转导:将力转化为生化信号。

Mechanotransduction involving multimodular proteins: converting force into biochemical signals.

作者信息

Vogel Viola

机构信息

Laboratory for Biologically Oriented Materials, Department of Materials, Swiss Federal Institute of Technology, ETH Zurich, CH-8093 Switzerland.

出版信息

Annu Rev Biophys Biomol Struct. 2006;35:459-88. doi: 10.1146/annurev.biophys.35.040405.102013.

DOI:10.1146/annurev.biophys.35.040405.102013
PMID:16689645
Abstract

Cells can sense and transduce a broad range of mechanical forces into distinct sets of biochemical signals that ultimately regulate cellular processes, including adhesion, proliferation, differentiation, and apoptosis. Deciphering at the nanoscale the design principles by which sensory elements are integrated into structural protein motifs whose conformations can be switched mechanically is crucial to understand the process of transduction of force into biochemical signals that are then integrated to regulate mechanoresponsive pathways. While the major focus in the search for mechanosensory units has been on membrane proteins such as ion channels, integrins, and associated cytoplasmic complexes, a multimodular design of tandem repeats of various structural motifs is ubiquitously found among extracellular matrix proteins, as well as cell adhesion molecules, and among many intracellular players that physically link transmembrane proteins to the contractile cytoskeleton. Single-molecule studies have revealed an unexpected richness of mechanosensory motifs, including force-regulated conformational changes of loop-exposed molecular recognition sites, intermediate states in the unraveling pathway that might either expose cryptic binding or phosphorylation sites, or regions that display enzymatic activity only when unmasked by force. Insights into mechanochemical signal conversion principles will also affect various technological fields, from biotechnology to tissue engineering and drug development.

摘要

细胞能够感知广泛的机械力,并将其转化为不同的生化信号集,这些信号最终调节细胞过程,包括黏附、增殖、分化和凋亡。在纳米尺度上解读感觉元件如何整合到其构象可通过机械方式切换的结构蛋白基序中的设计原则,对于理解力转化为生化信号然后整合以调节机械响应途径的过程至关重要。虽然寻找机械感觉单元的主要重点一直是膜蛋白,如离子通道、整合素和相关的细胞质复合物,但在细胞外基质蛋白、细胞黏附分子以及许多将跨膜蛋白与收缩性细胞骨架物理连接的细胞内成分中,普遍发现了各种结构基序串联重复的多模块设计。单分子研究揭示了机械感觉基序出人意料的丰富性,包括环暴露分子识别位点的力调节构象变化、解链途径中的中间状态,这些中间状态可能会暴露隐蔽的结合或磷酸化位点,或者是仅在被力揭开时才显示酶活性的区域。对机械化学信号转换原理的深入了解也将影响从生物技术到组织工程和药物开发等各个技术领域。

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