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Mixed Extracellular Matrix Ligands Synergistically Modulate Integrin Adhesion and Signaling

机译:混合细胞外基质配体协同调节整合素的粘附和信号传导。

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摘要

Cell adhesion to extracellular matrix (ECM) components through cell-surface integrin receptors is essential to the formation, maintenance and repair of numerous tissues, and therefore represents a central theme in the design of bioactive materials that successfully interface with the body. While the adhesive responses associated with a single ligand have been extensively analyzed, the effects of multiple integrin subtypes binding to multivalent ECM signals remain poorly understood. In the present study, we generated a high throughput platform of non-adhesive surfaces presenting well-defined, independent densities of two integrin-specific engineered ligands for the type I collagen (COL-I) receptor α2β1 and the fibronectin (FN) receptor α5β1 to evaluate the effects of integrin cross-talk on adhesive responses. Engineered surfaces displayed ligand density-dependent adhesive effects, and mixed ligand surfaces significantly enhanced cell adhesion strength and focal adhesion assembly compared to single FN and COL-I ligand surfaces. Moreover, surfaces presenting mixed COL-I/FN ligands synergistically enhanced FAK activation compared to the single ligand substrates. The enhanced adhesive activities of the mixed ligand surfaces also promoted elevated proliferation rates. Our results demonstrate interplay between multivalent ECM ligands in adhesive responses and downstream cellular signaling.
机译:细胞通过细胞表面整联蛋白受体与细胞外基质(ECM)组分的粘附对于许多组织的形成,维持和修复至关重要,因此代表了与人体成功对接的生物活性材料设计的中心主题。虽然已广泛分析了与单个配体相关的粘附反应,但对多整合素亚型与多价ECM信号结合的影响仍然知之甚少。在本研究中,我们生成了一个非粘合表面的高通量平台,该表面呈现出两种类型I胶原蛋白(COL-1)受体α2β1和纤连蛋白(FN)受体α5β1的整合素特异性工程配体的定义明确的独立密度评估整联蛋白串扰对黏附反应的影响。工程化表面显示出依赖于配体密度的粘合效果,并且与单个FN和COL-1配体表面相比,混合的配体表面显着增强了细胞的粘合强度和粘着力。而且,与单一配体底物相比,呈现出混合的COL-1 / FN配体的表面协同增强了FAK活化。混合的配体表面增强的粘合活性也促进了增殖速率的提高。我们的结果证明了多价ECM配体之间的黏附反应和下游细胞信号之间的相互作用。

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