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原肌球蛋白的结构域 12 至 16 通过与糖胺聚糖以及整合素 αV 和 α5β1 的相互作用促进细胞黏附和铺展。

Domains 12 to 16 of tropoelastin promote cell attachment and spreading through interactions with glycosaminoglycan and integrins alphaV and alpha5beta1.

机构信息

Department of Science, University of Basilicata, Potenza, Italy.

Charles Perkins Centre, The University of Sydney, NSW, Australia.

出版信息

FEBS J. 2021 Jul;288(13):4024-4038. doi: 10.1111/febs.15702. Epub 2021 Jan 26.

Abstract

Elastin is an extracellular matrix component with key structural and biological roles in elastic tissues. Interactions between resident cells and tropoelastin, the monomer of elastin, underpin elastin's regulation of cellular processes. However, the nature of tropoelastin-cell interactions and the contributions of individual tropoelastin domains to these interactions are only partly elucidated. In this study, we identified and characterized novel cell-adhesive sites in the tropoelastin N-terminal region between domains 12 and 16. We found that this region interacts with αV and α5β1 integrin receptors, which mediate cell attachment and spreading. A peptide sequence from within this region, spanning domains 14 to mid-domain 16, binds heparan sulfate through electrostatic interactions with peptide lysine residues and induces conformational ordering of the peptide. We propose that domains 14-16 direct initial cell attachment through cell-surface heparan sulfate glycosaminoglycans, followed by αV and α5β1 integrin-promoted attachment and spreading on domains 12-16 of tropoelastin. These findings advance our mechanistic understanding of elastin matrix biology, with the potential to enhance tissue regenerative outcomes of elastin-based materials.

摘要

弹性蛋白是细胞外基质的组成部分,在弹性组织中具有关键的结构和生物学功能。驻留细胞与弹性蛋白单体原弹性蛋白之间的相互作用是弹性蛋白调节细胞过程的基础。然而,原弹性蛋白与细胞的相互作用的性质以及各个原弹性蛋白结构域对这些相互作用的贡献仅部分阐明。在这项研究中,我们在 12 到 16 结构域之间的原弹性蛋白 N 端区域鉴定并表征了新的细胞黏附位点。我们发现该区域与介导细胞附着和扩展的αV 和α5β1 整合素受体相互作用。该区域内的一个肽序列,跨越结构域 14 到中结构域 16,通过与肽赖氨酸残基的静电相互作用与肝素硫酸盐结合,并诱导肽的构象有序化。我们提出,结构域 14-16 通过细胞表面肝素硫酸盐糖胺聚糖引导初始细胞附着,然后通过αV 和α5β1 整合素促进对原弹性蛋白的 12-16 结构域的附着和扩展。这些发现推进了我们对弹性蛋白基质生物学的机制理解,有可能增强基于弹性蛋白的材料的组织再生效果。

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