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PNAS Plus: Perfusable branching microvessel bed for vascularization of engineered tissues

机译:PNAS Plus:可灌注分支微血管床用于工程组织的血管形成

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摘要

Vascularization is critical for the survival of engineered tissues in vitro and in vivo. In vivo, angiogenesis involves endothelial cell proliferation and sprouting followed by connection of extended cellular processes and subsequent lumen propagation through vacuole fusion. We mimicked this process in engineering an organized capillary network anchored by an artery and a vein. The network was generated by inducing directed capillary sprouting from vascular explants on micropatterned substrates containing thymosin β4-hydrogel. The capillary outgrowths connected between the parent explants by day 21, a process that was accelerated to 14 d by application of soluble VEGF and hepatocyte growth factor. Confocal microscopy and transmission electron microscopy indicated the presence of tubules with lumens formed by endothelial cells expressing CD31, VE-cadherin, and von Willebrand factor. Cardiac tissues engineered around the resulting vasculature exhibited improved functional properties, cell striations, and cell–cell junctions compared with tissues without prevascularization. This approach uniquely allows easy removal of the vasculature from the microfabricated substrate and easy seeding of the tissue specific cell types in the parenchymal space.
机译:血管化对于工程组织在体外和体内的存活至关重要。在体内,血管生成涉及内皮细胞的增殖和发芽,随后是延伸的细胞过程的连接以及随后通过液泡融合的管腔繁殖。我们在设计一个由动脉和静脉锚定的有组织的毛细管网络时模仿了这一过程。该网络是通过在含胸腺素β4-水凝胶的微图案化底物上诱导血管外植体产生定向毛细血管生成的。到第21天,亲本外植体之间的毛细血管生长相连,这一过程通过应用可溶性VEGF和肝细胞生长因子而加速至14天。共聚焦显微镜和透射电镜表明存在表达CD31,VE-钙粘着蛋白和von Willebrand因子的内皮细胞形成管腔的小管。与没有血管形成的组织相比,围绕所得脉管系统工程改造的心脏组织表现出改善的功能特性,细胞条纹和细胞间连接。该方法独特地允许容易地从微加工的基底去除脉管系统,并且容易地将组织特异性细胞类型播种在实质空间中。

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