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Physical and Chemical Signals That Promote Vascularization of Capillary-Scale Channels

机译:促进毛细血管通道血管化的物理和化学信号

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摘要

Proper vascularization remains critical to the clinical application of engineered tissues. To engineer microvessels in vitro, we and others have delivered endothelial cells through preformed channels into patterned extracellular matrix-based gels. This approach has been limited by the size of endothelial cells in suspension, and results in plugging of channels below ~30 μm in diameter. Here, we examine physical and chemical signals that can augment direct seeding, with the aim of rapidly vascularizing capillary-scale channels. By studying tapered microchannels in type I collagen gels under various conditions, we establish that stiff scaffolds, forward pressure, and elevated cyclic AMP levels promote endothelial stability and that reverse pressure promotes endothelial migration. We applied these results to uniform 20-μm-diameter channels and optimized the magnitudes of pressure, flow, and shear stress to best support endothelial migration and vascular stability. This vascularization strategy is able to form millimeter-long perfusable capillaries within three days. Our results indicate how to manipulate the physical and chemical environment to promote rapid vascularization of capillary-scale channels within type I collagen gels.
机译:正确的血管形成对于工程组织的临床应用仍然至关重要。为了在体外工程化微血管,我们和其他公司已经通过预先形成的通道将内皮细胞递送到图案化的基于细胞外基质的凝胶中。该方法受到悬浮液中内皮细胞大小的限制,并导致直径小于约30μm的通道堵塞。在这里,我们研究了可以增加直接播种的物理和化学信号,目的是快速血管化毛细血管通道。通过研究各种条件下I型胶原蛋白凝胶中的锥形微通道,我们发现刚性支架,正向压力和升高的环AMP含量可促进内皮稳定性,而反向压力则可促进内皮迁移。我们将这些结果应用到直径为20μm的均匀通道上,并优化了压力,流量和剪切应力的大小,以最佳地支持内皮迁移和血管稳定性。这种血管化策略能够在三天内形成毫米长的可灌注毛细血管。我们的结果表明如何操纵物理和化学环境以促进I型胶原蛋白凝胶内毛细血管通道的快速血管化。

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