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含氨基酸基扩链剂的可降解嵌段聚氨酯的体外降解与侵蚀

In vitro degradation and erosion of degradable, segmented polyurethanes containing an amino acid-based chain extender.

作者信息

Skarja G A, Woodhouse K A

机构信息

Department of Chemical Engineering and Applied Chemistry, University of Toronto, Ontario, Canada.

出版信息

J Biomater Sci Polym Ed. 2001;12(8):851-73. doi: 10.1163/156856201753113060.

Abstract

In vitro degradation and erosion of novel, degradable segmented polyurethanes containing a phenylalanine diester chain extender were investigated by exposing the polymers to buffer. chymotrypsin, and trypsin solutions for up to 28 days. Polyurethane degradation and erosion were monitored by gravimetry, scanning electron microscopy (SEM), and gel permeation chromatography (GPC) and compared to a control polyurethane. Polyurethanes were synthesized using two different soft segments (polycaprolactone diol and polyethylene oxide) of variable molecular weight. Inclusion of the phenylalanine-based chain extender resulted in an increased susceptibility to enzyme-mediated, but not buffer-mediated, erosion in comparison to the control polyurethane. SEM analysis indicated that enzyme-mediated erosion proceeded via a surface-limited mechanism resulting in a progressive removal of material from the surface inwards with time. The magnitude of degradation and erosion was highly variable and was dependent on soft segment type and molecular weight. The range of degradation rates, as well as physicochemical properties, makes these polyurethanes potentially useful for a wide range of biomedical applications.

摘要

通过将含有苯丙氨酸二酯扩链剂的新型可降解嵌段聚氨酯暴露于缓冲液、胰凝乳蛋白酶和胰蛋白酶溶液中长达28天,对其体外降解和侵蚀情况进行了研究。通过重量法、扫描电子显微镜(SEM)和凝胶渗透色谱法(GPC)监测聚氨酯的降解和侵蚀情况,并与对照聚氨酯进行比较。使用两种不同分子量的软段(聚己内酯二醇和聚环氧乙烷)合成聚氨酯。与对照聚氨酯相比,含苯丙氨酸的扩链剂导致对酶介导的侵蚀(而非缓冲液介导的侵蚀)的敏感性增加。SEM分析表明,酶介导的侵蚀通过表面受限机制进行,导致材料随时间从表面向内逐渐去除。降解和侵蚀的程度变化很大,并且取决于软段类型和分子量。降解速率范围以及物理化学性质使这些聚氨酯在广泛的生物医学应用中具有潜在用途。

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