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Designer artificial membrane binding proteins to direct stem cells to the myocardium

机译:设计人工膜结合蛋白将干细胞引导至心肌

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摘要

We present a new cell membrane modification methodology where the inherent heart tissue homing properties of the infectious bacteria Streptococcus gordonii are transferred to human stem cells. This is achieved via the rational design of a chimeric protein–polymer surfactant cell membrane binding construct, comprising the cardiac fibronectin (Fn) binding domain of the bacterial adhesin protein CshA fused to a supercharged protein. Significantly, the protein–polymer surfactant hybrid spontaneously inserts into the plasma membrane of stem cells without cytotoxicity, instilling the cells with a high affinity for immobilized fibronectin. Moreover, we show that this cell membrane reengineering approach significantly improves retention and homing of stem cells delivered either intracardially or intravenously to the myocardium in a mouse model.
机译:我们提出了一种新的细胞膜修饰方法,其中传染性细菌戈登链球菌的固有心脏组织归巢特性被转移到人干细胞。这是通过对嵌合蛋白与聚合物表面活性剂细胞膜结合构建物进行合理设计而实现的,该构建物包含与粘附蛋白融合的细菌粘附素蛋白CshA的心脏纤连蛋白(Fn)结合域。值得注意的是,蛋白质-聚合物表面活性剂杂合物自发地插入干细胞的质膜中,而没有细胞毒性,使细胞对固定的纤连蛋白具有高亲和力。此外,我们表明,这种细胞膜再造方法可显着改善在小鼠模型中通过心内或静脉内递送至心肌的干细胞的保留和归巢。

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