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早期粘着斑形成过程中整合素与细丝蛋白的结合机制及其与踝蛋白的相互作用。

Mechanisms of integrin and filamin binding and their interplay with talin during early focal adhesion formation.

作者信息

Truong Tiffany, Shams Hengameh, Mofrad Mohammad R K

机构信息

Molecular Cell Biomechanics Laboratory, Departments of Bioengineering and Mechanical Engineering, University of California Berkeley, 208A Stanley Hall #1762, Berkeley, CA 94704-1762, USA.

出版信息

Integr Biol (Camb). 2015 Oct;7(10):1285-96. doi: 10.1039/c5ib00133a. Epub 2015 Jul 9.

Abstract

Filamin plays a key role in cellular biomechanics as an actin cross-linker and as a versatile focal adhesion binding partner. It binds directly to integrins, a family of mechanosensitive transmembrane receptors that mediate attachment to several extracellular ligands such as fibronectin, collagen, and laminin. Filamin binds β-integrin at its cytoplasmic tail, competing with talin, a major integrin activator that plays a chief role in cell adhesion. Herein, we develop molecular dynamics models to study the mechanism of early binding of αIIbβ3 integrin with filamin A (FLNa). Our models predict three important electrostatic interactions and one stabilizing hydrophobic interaction that mediate binding between filamin and integrin. In its native conformation, filamin's integrin binding site is auto-inhibited. Our models help shed light on the role of integrin binding on regulating filamin activation. Finally, the effect of talin on the filamin-integrin interaction is explored and possible scenarios of the interplay among these molecules are examined.

摘要

细丝蛋白作为肌动蛋白交联剂和多功能黏着斑结合伴侣,在细胞生物力学中发挥关键作用。它直接与整合素结合,整合素是一类机械敏感的跨膜受体家族,介导细胞与多种细胞外配体如纤连蛋白、胶原蛋白和层粘连蛋白的附着。细丝蛋白在其细胞质尾部结合β整合素,与踝蛋白竞争,踝蛋白是一种主要的整合素激活剂,在细胞黏附中起主要作用。在此,我们开发分子动力学模型来研究αIIbβ3整合素与细丝蛋白A(FLNa)早期结合的机制。我们的模型预测了三种重要的静电相互作用和一种稳定的疏水相互作用,这些相互作用介导了细丝蛋白与整合素之间的结合。在其天然构象中,细丝蛋白的整合素结合位点被自身抑制。我们的模型有助于阐明整合素结合在调节细丝蛋白激活中的作用。最后,研究了踝蛋白对细丝蛋白 - 整合素相互作用的影响,并探讨了这些分子之间相互作用的可能情况。

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