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Artificial cell membrane binding thrombin constructs drive in situ fibrin hydrogel formation

机译:人工细胞膜结合凝血酶构建物驱动原位纤维蛋白水凝胶形成

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摘要

Cell membrane re-engineering is emerging as a powerful tool for the development of next generation cell therapies, as it allows the user to augment therapeutic cells to provide additional functionalities, such as homing, adhesion or hypoxia resistance. To date, however, there are few examples where the plasma membrane is re-engineered to display active enzymes that promote extracellular matrix protein assembly. Here, we report on a self-contained matrix-forming system where the membrane of human mesenchymal stem cells is modified to display a novel thrombin construct, giving rise to spontaneous fibrin hydrogel nucleation and growth at near human plasma concentrations of fibrinogen. The cell membrane modification process is realised through the synthesis of a membrane-binding supercationic thrombin-polymer surfactant complex. Significantly, the resulting robust cellular fibrin hydrogel constructs can be differentiated down osteogenic and adipogenic lineages, giving rise to self-supporting monoliths that exhibit Young’s moduli that reflect their respective extracellular matrix compositions.
机译:细胞膜再造正在成为开发下一代细胞疗法的有力工具,因为它允许用户增加治疗细胞以提供其他功能,例如归巢,粘附或耐缺氧性。然而,迄今为止,很少有例子对质膜进行改造,以展示促进细胞外基质蛋白组装的活性酶。在这里,我们报告一个自成体系的基质形成系统,其中人间充质干细胞的膜被修饰以显示新型的凝血酶构建体,在接近人血浆中的纤维蛋白原浓度下产生自发性纤维蛋白水凝胶成核和生长。细胞膜修饰过程是通过膜结合的超阳离子凝血酶-聚合物表面活性剂复合物的合成来实现的。重要的是,可以将得到的坚固的细胞纤维蛋白水凝胶构建体分化为成骨和成脂谱系,从而产生具有杨氏模量的自支撑整体,反映了它们各自的细胞外基质组成。

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