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组织工程血管移植物在动脉循环中不断演变的生物力学特性的表征

Characterization of evolving biomechanical properties of tissue engineered vascular grafts in the arterial circulation.

作者信息

Udelsman Brooks V, Khosravi Ramak, Miller Kristin S, Dean Ethan W, Bersi Matthew R, Rocco Kevin, Yi Tai, Humphrey Jay D, Breuer Christopher K

机构信息

Yale University School of Medicine, 10 Amistad Street, New Haven, CT 06519, USA.

Yale School of Engineering and Applied Science, 55 Prospect Street, New Haven, CT 06520, USA.

出版信息

J Biomech. 2014 Jun 27;47(9):2070-9. doi: 10.1016/j.jbiomech.2014.03.011. Epub 2014 Mar 15.

Abstract

We used a murine model to assess the evolving biomechanical properties of tissue engineered vascular grafts (TEVGs) implanted in the arterial circulation. The initial polymeric tubular scaffold was fabricated from poly(lactic acid)(PLA) and coated with a 50:50 copolymer of poly(caprolactone) and poly(lactic acid)(P[PC/LA]). Following seeding with syngeneic bone marrow derived mononuclear cells, TEVGs (n=50) were implanted as aortic interposition grafts in wild-type mice and monitored serially using ultrasound. A custom biaxial mechanical testing device was used to quantify the in vitro circumferential and axial mechanical properties of grafts explanted at 3 or 7 months. At both times, TEVGs were much stiffer than native tissue in both directions. Repeated mechanical testing of some TEVGs treated with elastase or collagenase suggested that elastin did not contribute significantly to the overall stiffness whereas collagen did contribute. Traditional histology and immunostaining revealed smooth muscle cell layers, significant collagen deposition, and increasing elastin production in addition to considerable scaffold at both 3 and 7 months, which likely dominated the high stiffness seen in mechanical testing. These results suggest that PLA has inadequate in vivo degradation, which impairs cell-mediated development of vascular neotissue having properties closer to native arteries. Assessing contributions of individual components, such as elastin and collagen, to the developing neovessel is needed to guide computational modeling that may help to optimize the design of the TEVG.

摘要

我们使用小鼠模型来评估植入动脉循环中的组织工程血管移植物(TEVG)不断演变的生物力学特性。最初的聚合物管状支架由聚乳酸(PLA)制成,并涂覆有聚己内酯和聚乳酸的50:50共聚物(P[PC/LA])。在用同基因骨髓来源的单核细胞接种后,将50个TEVG作为主动脉间置移植物植入野生型小鼠体内,并使用超声进行连续监测。使用定制的双轴机械测试装置来量化在3个月或7个月时取出的移植物的体外周向和轴向力学性能。在这两个时间点,TEVG在两个方向上都比天然组织硬得多。对一些用弹性蛋白酶或胶原酶处理的TEVG进行重复机械测试表明,弹性蛋白对整体硬度的贡献不大,而胶原蛋白有贡献。传统组织学和免疫染色显示,在3个月和7个月时,除了大量支架外,还有平滑肌细胞层、大量胶原蛋白沉积和弹性蛋白生成增加,这可能是机械测试中观察到的高硬度的主要原因。这些结果表明,PLA在体内的降解不足,这会损害细胞介导的具有更接近天然动脉特性的血管新组织的发育。需要评估弹性蛋白和胶原蛋白等单个成分对发育中的新血管的贡献,以指导计算建模,这可能有助于优化TEVG的设计。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0cb3/4747059/b5c4baecc06f/nihms581902f1.jpg

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