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Neomycin binding preserves extracellular matrix in bioprosthetic heart valves during in vitro cyclic fatigue and storage

机译:新霉素结合可在体外循环疲劳和存储过程中在生物人工心脏瓣膜中保存细胞外基质

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摘要

Bioprosthetic heart valve (BHV) cusps have a complex architecture consisting of an anisotropic arrangement of collagen, glycosaminoglycans (GAGs) and elastin. Glutaraldehyde (GLUT) is used as a fixative for all clinical BHV implants; however, it only stabilizes the collagen component of the tissue, and other components such as GAGs and elastin are lost from the tissue during processing, storage or after implantation. We have shown previously that the effectiveness of the chemical crosslinking can be increased by incorporating neomycin trisulfate, a hyaluronidase inhibitor, to prevent the enzyme-mediated GAG degradation. In the present study, we optimized carbodiimide-based GAG-targeted chemistry to incorporate neomycin into BHV cusps prior to conventional GLUT crosslinking. This crosslinking leads to enhanced preservation of GAGs during in vitro cyclic fatigue and storage. The neomycin group showed greater GAG retention after both 10 and 50 million accelerated-fatigue cycles and after 1 year of storage in GLUT solution. Thus, additional binding of neomycin to the cusps prior to standard GLUT crosslinking could enhance tissue stability and thus heart valve durability.
机译:生物人工心脏瓣膜(BHV)尖端具有复杂的结构,由胶原蛋白,糖胺聚糖(GAG)和弹性蛋白的各向异性排列组成。戊二醛(GLUT)被用作所有临床BHV植入物的固定剂。但是,它只能稳定组织的胶原蛋白成分,在加工,存储或植入后,其他成分(例如GAG和弹性蛋白)会从组织中流失。先前我们已经表明,可以通过加入新霉素三硫酸盐(一种透明质酸酶抑制剂)来提高化学交联的有效性,以防止酶介导的GAG降解。在本研究中,我们优化了基于碳二亚胺的GAG靶向化学,以在常规GLUT交联之前将新霉素掺入BHV牙尖。这种交联导致GAG在体外循环疲劳和存储过程中的保存增强。新霉素组在10和5千万个加速疲劳周期后以及在GLUT溶液中保存1年后显示出更高的GAG保留率。因此,在标准的GLUT交联之前,新霉素与针尖的额外结合可以增强组织稳定性,从而增强心脏瓣膜的耐用性。

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