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Collagen scaffolds functionalized with triple-helical peptides support 3D HUVEC culture

机译:用三螺旋肽官能化的胶原蛋白支架支持3D Huvec文化

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摘要

Porous biomaterials which provide a structural and biological support for cells have immense potential in tissue engineering and cell-based therapies for tissue repair. Collagen biomaterials that can host endothelial cells represent promising tools for the vascularization of engineered tissues. Three-dimensional collagen scaffolds possessing controlled architecture and mechanical stiffness are obtained through freeze–drying of collagen suspensions, followed by chemical cross-linking which maintains their stability. However, cross-linking scaffolds renders their biological activity suboptimal for many cell types, including human umbilical vein endothelial cells (HUVECs), by inhibiting cell–collagen interactions. Here, we have improved crucial HUVEC interactions with such cross-linked collagen biomaterials by covalently coupling combinations of triple-helical peptides (THPs). These are ligands for collagen-binding cell-surface receptors (integrins or discoidin domain receptors) or secreted proteins (SPARC and von Willebrand factor). THPs enhanced HUVEC adhesion, spreading and proliferation on 2D collagen films. THPs grafted to 3D-cross-linked collagen scaffolds promoted cell survival over seven days. This study demonstrates that THP-functionalized collagen scaffolds are promising candidates for hosting endothelial cells with potential for the production of vascularized engineered tissues in regenerative medicine applications.
机译:多孔生物材料,其为细胞提供结构和生物载体具有巨大的组织工程和基于细胞的组织修复疗法的潜力。胶原蛋白生物材料可以宿主内皮细胞代表工程组织的血管化的有希望的工具。通过胶原蛋白悬浮液的冷冻干燥获得具有受控结构和机械刚度的三维胶原屑支架,然后通过稳定性地进行化学交联。然而,通过抑制细胞 - 胶原蛋白相互作用,交联支架使其包括许多细胞类型的生物活性次优,包括人脐静脉内皮细胞(HUVECS)。这里,通过共价偶联三螺旋肽(THP),改善了与这种交联的胶原生物材料相互作用的关键与这种交联的胶原生物材料相互作用。这些是用于胶原结合细胞表面受体(整联蛋白或窝囊结构域受体)或分泌蛋白质(SPARC和VONERBLAND因子)的配体。 THP提高HUVEC粘附,扩散和增殖在2D胶原膜上。接枝到3D交联的胶原蛋白支架的THP促进了七天内的细胞生存。该研究表明,THP官能化的胶原蛋白支架是托管内皮细胞的候选者,其具有在再生医学应用中生产血管化工程组织的潜力。

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