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首页> 外文期刊>ACS nano >Aligned-Braided Nanofibrillar Scaffold with Endothelial Cells Enhances Arteriogenesis
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Aligned-Braided Nanofibrillar Scaffold with Endothelial Cells Enhances Arteriogenesis

机译:对齐编织的纳米纤维支架与内皮细胞增强动脉生成。

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The objective of this study was to enhance the angiogenic capacity of endothelial cells (ECs) using nanoscale signaling cues from aligned nanofibrillar scaffolds in the setting of tissue ischemia. Thread-like nanofibrillar scaffolds with porous structure were fabricated from aligned-braided membranes generated under shear from liquid crystal collagen solution. Human ECs showed greater outgrowth from aligned scaffolds than from nonpatterned scaffolds. Integrin alpha 1 was in part responsible for the enhanced cellular outgrowth on aligned nanofibrillar scaffolds, as the effect was abrogated by integrin a1 inhibition. To test the efficacy of EC-seeded aligned nanofibrillar scaffolds in improving neovascularization in vivo, the ischemic limbs of mice were treated with EC-seeded aligned nanofibrillar scaffold; EC-seeded nonpatterned scaffold; ECs in saline; aligned nanofibrillar scaffold alone; or no treatment. After 14 days, laser Doppler blood spectroscopy demonstrated significant improvement in blood perfusion recovery when treated with EC-seeded aligned nanofibrillar scaffolds, in comparison to ECs in saline or no treatment. In ischemic hindlimbs treated with scaffolds seeded with human ECs derived from induced pluripotent stem cells (iPSC-ECs), single-walled carbon nanotube (SWNT) fluorophores were systemically delivered to quantify microvascular density after 28 days. Near infrared-II (NIR-II, 1000-1700 nm) imaging of SWNT fluorophores demonstrated that iPSC-EC-seeded aligned scaffolds group showed significantly higher microvascular density than the saline or cells groups. These data suggest that treatment with EC-seeded aligned nanofibrillar scaffolds improved blood perfusion and arteriogenesis, when compared to treatment with cells alone or scaffold alone, and have important implications in the design of therapeutic cell delivery strategies.
机译:这项研究的目的是在组织缺血的情况下,使用来自对齐的纳米原纤维支架的纳米级信号提示来增强内皮细胞(EC)的血管生成能力。由液晶胶原溶液在剪切作用下产生的排列编织膜制成具有多孔结构的线状纳米原纤维支架。与没有图案的支架相比,与对齐的支架相比,人类EC的生长更大。整联蛋白α1部分负责对齐的纳米原纤维支架上的细胞生长增强,因为整联蛋白a1抑制作用消除了这种作用。为了测试EC接种的排列的纳米原纤维支架在体内改善新血管形成的功效,用EC接种的排列的纳米原纤维支架治疗小鼠的缺血肢体。 EC播种的无图案支架; ECs在盐水中;单独排列纳米纤维支架;或不治疗。 14天后,与生理盐水或未治疗的EC相比,激光多普勒血液光谱术显示当使用EC接种的对齐纳米原纤维支架治疗时,血液灌注恢复显着改善。在缺血性后肢中,植入由诱导多能干细胞(iPSC-EC)衍生的人EC的支架后,系统递送28天后的单壁碳纳米管(SWNT)荧光团以定量微血管密度。 SWNT荧光团的近红外II(NIR-II,1000-1700 nm)成像表明,iPSC-EC接种的对齐支架组显示的微血管密度明显高于生理盐水或细胞组。这些数据表明,与单独使用细胞或单独使用支架进行治疗相比,使用EC接种的对齐纳米原纤维支架进行治疗可改善血液灌注和动脉生成,并且对治疗性细胞递送策略的设计具有重要意义。

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