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通过改变基底结合的表皮生长因子的密度来调节整合素黏附。

Regulation of integrin adhesions by varying the density of substrate-bound epidermal growth factor.

机构信息

Department of Molecular Cell Biology, Weizmann Institute of Science, 76100, Rehovot, Israel.

出版信息

Biointerphases. 2012 Dec;7(1-4):23. doi: 10.1007/s13758-012-0023-0. Epub 2012 Mar 3.

Abstract

Substrates coated with specific bioactive ligands are important for tissue engineering, enabling the local presentation of extracellular stimulants at controlled positions and densities. In this study, we examined the cross-talk between integrin and epidermal growth factor (EGF) receptors following their interaction with surface-immobilized Arg-Gly-Asp (RGD) and EGF ligands, respectively. Surfaces of glass coverslips, modified with biotinylated silane-polyethylene glycol, were functionalized by either biotinylated RGD or EGF (or both) via the biotin-NeutrAvidin interaction. Fluorescent labeling of the adhering A431 epidermoid carcinoma cells for zyxin or actin indicated that EGF had a dual effect on focal adhesions (FA) and stress fibers: at low concentrations (0.1; 1 ng/ml), it stimulated their growth; whereas at higher concentrations, on surfaces with low to intermediate RGD densities, it induced their disassembly, leading to cell detachment. The EGF-dependent dissociation of FAs was, however, attenuated on higher RGD density surfaces. Simultaneous stimulation by both immobilized RGD and EGF suggest a strong synergy between integrin and EGFR signaling, in FA induction and cell spreading. A critical threshold level of EGF was required to induce significant variation in cell adhesion; beyond this critical density, the immobilized molecule had a considerably stronger effect on cell adhesion than did soluble EGF. The mechanisms underlying this synergy between the adhesion ligand and EGF are discussed.

摘要

用特定的生物活性配体涂覆的基底对于组织工程非常重要,使细胞外刺激物能够在受控位置和密度处局部呈现。在这项研究中,我们研究了整合素和表皮生长因子 (EGF) 受体在与表面固定的 Arg-Gly-Asp (RGD) 和 EGF 配体分别相互作用后的串扰。用生物素化硅烷-聚乙二醇修饰的玻璃盖玻片的表面通过生物素-NeutrAvidin 相互作用被生物素化的 RGD 或 EGF(或两者)功能化。用荧光标记黏附的 A431 表皮样癌细胞的 zyxin 或肌动蛋白表明,EGF 对焦点黏附(FA)和应力纤维有双重影响:在低浓度(0.1;1ng/ml)下,它刺激它们的生长;然而,在更高的浓度下,在低到中等 RGD 密度的表面上,它诱导它们解体,导致细胞脱落。然而,在更高的 RGD 密度表面上,EGF 依赖性 FA 解离被减弱。同时刺激固定的 RGD 和 EGF 表明整合素和 EGFR 信号之间存在强烈的协同作用,在 FA 诱导和细胞扩展中。需要 EGF 的临界阈值水平来引起细胞黏附的显著变化;超过这个临界密度,固定分子对细胞黏附的影响比可溶性 EGF 强得多。讨论了这种黏附配体和 EGF 之间协同作用的机制。

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