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静水压独立增加小直径工程化动脉构建体中弹性蛋白和胶原蛋白的共表达。

Hydrostatic pressure independently increases elastin and collagen co-expression in small-diameter engineered arterial constructs.

机构信息

Department of Surgery and the McGowan Institute for Regenerative Medicine, University of Pittsburgh, 450 Technology Drive, Suite 300, Pittsburgh, Pennsylvania 15219, USA.

出版信息

J Biomed Mater Res A. 2011 Mar 15;96(4):673-81. doi: 10.1002/jbm.a.33019. Epub 2011 Jan 25.

Abstract

Prior studies have demonstrated that smooth muscle cell (SMC) proliferation, migration, and extracellular matrix production increase with hydrostatic pressure in vitro. We have engineered highly compliant small-diameter arterial constructs by culturing primary adult baboon arterial SMCs under pulsatile perfusion on tubular, porous, elastomeric scaffolds composed of poly(glycerol sebacate) (PGS). This study investigates the effect of hydrostatic pressure on the biological and mechanical properties of PGS-based engineered arterial constructs. Pressure was raised using a downstream needle valve during perfusion while preserving flow rate and pulsatility, and constructs were evaluated by pressure-diameter testing and biochemical assays for collagen and elastin. Pressurized constructs contained half as much insoluble elastin as baboon common carotid arteries but were significantly less compliant, while constructs cultured at low hydrostatic pressure contained one-third as much insoluble elastin as baboon carotids and were similar in compliance. Hydrostatic pressure significantly increased construct burst pressure, collagen and insoluble elastin content, and soluble elastin concentration in culture medium. All arteries and constructs exhibited elastic recovery during pressure cycling. Hydrostatic pressure did not appear to affect radial distribution of SMCs, collagens I and III, and elastin. These results provide insights into the control of engineered smooth muscle tissue properties using hydrostatic pressure.

摘要

先前的研究已经表明,平滑肌细胞(SMC)的增殖、迁移和细胞外基质的产生会随着体外静水压力的增加而增加。我们通过在管状多孔弹性支架上对原代成年狨猴动脉 SMC 进行搏动灌注培养,构建了高顺应性小直径动脉构建体,该支架由聚(癸二酸甘油酯)(PGS)组成。本研究探讨了静水压力对基于 PGS 的工程化动脉构建体的生物学和机械性能的影响。在保持流量和脉动性的同时,通过在灌注过程中使用下游针阀来增加压力,通过压力-直径测试和胶原和弹性蛋白的生化分析来评估构建体。加压构建体中不溶性弹性蛋白含量仅为狨猴颈总动脉的一半,但顺应性显著降低,而在低静水压力下培养的构建体中不溶性弹性蛋白含量仅为狨猴颈动脉的三分之一,顺应性相似。静水压力显著增加了构建体的爆裂压力、胶原和不溶性弹性蛋白含量以及培养基中可溶性弹性蛋白的浓度。所有动脉和构建体在压力循环过程中均表现出弹性恢复。静水压力似乎不会影响 SMC、I 型和 III 型胶原以及弹性蛋白的径向分布。这些结果为使用静水压力控制工程化平滑肌组织特性提供了深入了解。

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