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新型霉素和五倍子酰葡萄糖增强交联以保存生物人工心脏瓣膜中的弹性蛋白和糖胺聚糖。

Neomycin and pentagalloyl glucose enhanced cross-linking for elastin and glycosaminoglycans preservation in bioprosthetic heart valves.

机构信息

Cardiovascular Implant Research Laboratory, Department of Bioengineering, Clemson University, Clemson, SC, USA.

出版信息

J Biomater Appl. 2014 Jan;28(5):757-66. doi: 10.1177/0885328213479047.

Abstract

Glutaraldehyde cross-linked bioprosthetic heart valves fail within 12-15 years of implantation due to limited durability. Glutaraldehyde does not adequately stabilize extracellular matrix components such as glycosaminoglycans and elastin, and loss of these components could be a major cause of degeneration of valve after implantation. We have shown earlier that neomycin-based cross-linking stabilizes glycosaminoglycans in the tissue but fails to stabilize elastin component. Here, we report a new treatment where neomycin and pentagalloyl glucose (PGG) were incorporated into glutaraldehyde cross-linking neomycin-PGG-Glutaraldehyde (NPG) to stabilize both glycosaminoglycans and elastin in porcine aortic valves. In vitro studies demonstrated a marked increase in extracellular matrix stability against enzymatic degradation after cross-linking and 10 month storage in NPG group when compared to glutaraldehyde controls. Tensile properties showed increased lower elastic modulus in both radial and circumferential directions in NPG group as compared to glutaraldehyde, probably due to increased elastin stabilization with no changes in upper elastic modulus and extensibility. The enhanced extracellular matrix stability was further maintained in NPG-treated tissues after rat subdermal implantation for three weeks. NPG group also showed reduced calcification when compared to glutaraldehyde controls. We conclude that NPG cross-linking would be an excellent alternative to glutaraldehyde cross-linking of bioprosthetic heart valves to improve its durability.

摘要

戊二醛交联生物瓣在植入 12-15 年后因耐久性有限而失效。戊二醛不能充分稳定细胞外基质成分,如糖胺聚糖和弹性蛋白,这些成分的丢失可能是植入后瓣膜退化的主要原因。我们之前已经表明,基于新霉素的交联可以稳定组织中的糖胺聚糖,但不能稳定弹性蛋白成分。在这里,我们报告了一种新的治疗方法,即将新霉素和五没食子酰葡萄糖(PGG)纳入戊二醛交联新霉素-PGG-戊二醛(NPG)中,以稳定猪主动脉瓣中的糖胺聚糖和弹性蛋白。体外研究表明,与戊二醛对照组相比,交联后和 NPG 组 10 个月储存后的细胞外基质稳定性对酶降解有明显增加。与戊二醛相比,NPG 组的径向和环向拉伸性能的下弹性模量均增加,这可能是由于弹性蛋白稳定性增加,而上弹性模量和延伸率没有变化。在大鼠皮下植入三周后,NPG 处理的组织中的细胞外基质稳定性进一步保持。与戊二醛对照组相比,NPG 组的钙化也减少。我们得出结论,NPG 交联将是生物瓣戊二醛交联的极好替代方法,以提高其耐久性。

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