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Interface Immobilization Chemistry of c RGD-based Peptides Regulates Integrin Mediated Cell Adhesion

机译:基于c RGD的肽的界面固定化化学调节整合素介导的细胞粘附。

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摘要

The interaction of specifi c surface receptors of the integrin family with different extracellular matrix-based ligands is of utmost importance for the cellular adhesion process. A ligand consists of an integrin-binding group, here cyclic RGDfX, a spacer molecule that lifts the integrin-binding group from the surface and a surface anchoring group. c (-RGDfX-) peptides are bound to gold nanoparticle structured surfaces via polyproline, polyethylene glycol or aminohexanoic acid containing spacers of different lengths. Although keeping the integrin-binding c (-RGDfX-) peptides constant for all compounds, changes of the ligand´s spacer chemistry and length reveal signifi cant differences in cell adhesion activation and focal adhesion formation. Polyproline-based peptides demonstrate improved cell adhesion kinetics and focal adhesion formation compared with common aminohexanoic acid or polyethylene glycol spacers. Binding activity can additionally be improved by applying ligands with two head groups, inducing a multimeric effect. This study gives insights into spacer-based differences in integrin-driven cell adhesion processes and remarkably highlights the polyproline-based spacers as suitable ligand-presenting templates for surface functionalization.
机译:整联蛋白家族的特定表面受体与不同的基于细胞外基质的配体之间的相互作用对于细胞粘附过程至关重要。配体由整联蛋白结合基团(此处为环状RGDfX),从表面提起整联蛋白结合基团的间隔分子和表面锚定基团组成。 c(-RGDfX-)肽通过聚脯氨酸,聚乙二醇或含不同长度间隔基的氨基己酸与金纳米颗粒结构化表面结合。尽管对于所有化合物而言,整合素结合性c(-RGDfX-)肽均保持恒定,但配体间隔基化学性质和长度的变化显示出细胞粘附激活和黏着斑形成的显着差异。与普通的氨基己酸或聚乙二醇间隔基相比,基于聚脯氨酸的肽表现出改善的细胞粘附动力学和粘着斑形成。通过施加具有两个头基的配体,还可以提高结合活性,从而诱导多聚效应。这项研究深入了解了整合素驱动的细胞粘附过程中基于间隔基的差异,并显着强调了基于聚脯氨酸的间隔基作为表面功能化的合适的配体表现模板。

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