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Geometric control of vascular networks to enhance engineered tissue integration and function

机译:血管网络的几何控制以增强工程组织的整合和功能

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摘要

Tissue vascularization and integration with host circulation remains a key barrier to the translation of engineered tissues into clinically relevant therapies. Here, we used a microtissue molding approach to demonstrate that constructs containing highly aligned “cords” of endothelial cells triggered the formation of new capillaries along the length of the patterned cords. These vessels became perfused with host blood as early as 3 d post implantation and became progressively more mature through 28 d. Immunohistochemical analysis showed that the neovessels were composed of human and mouse endothelial cells and exhibited a mature phenotype, as indicated by the presence of alpha-smooth muscle actin–positive pericytes. Implantation of cords with a prescribed geometry demonstrated that they provided a template that defined the neovascular architecture in vivo. To explore the utility of this geometric control, we implanted primary rat and human hepatocyte constructs containing randomly organized endothelial networks vs. ordered cords. We found substantially enhanced hepatic survival and function in the constructs containing ordered cords following transplantation in mice. These findings demonstrate the importance of multicellular architecture in tissue integration and function, and our approach provides a unique strategy to engineer vascular architecture.
机译:组织血管化和与宿主循环的整合仍然是将工程组织转化为临床相关疗法的主要障碍。在这里,我们使用微组织成型方法来证明含有高度对齐的内皮细胞“帘线”的构建体会沿着图案化的帘线的长度触发新的毛细血管的形成。这些血管早在植入后3天就被宿主血液灌注,并在28天后逐渐成熟。免疫组织化学分析显示,新生血管由人和小鼠的内皮细胞组成,并表现出成熟的表型,如α-平滑肌肌动蛋白阳性周细胞的存在所表明。具有规定几何形状的脐带植入表明,它们提供了定义体内新血管结构的模板。为了探索这种几何控制的效用,我们植入了包含随机组织的内皮网络与有序脐带的大鼠和人肝细胞原代结构。我们发现,在小鼠体内移植后,含有有序脐带的构建体中的肝存活和功能大大增强。这些发现证明了多细胞结构在组织整合和功能中的重要性,我们的方法为工程血管结构提供了独特的策略。

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