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具有聚环氧乙烷表面改性端基的聚醚聚氨酯的体内生物稳定性;抗生物氧化和应力开裂性能。

In vivo biostability of polyether polyurethanes with polyethylene oxide surface-modifying end groups; resistance to biologic oxidation and stress cracking.

作者信息

Ebert Mike, Ward Bob, Anderson James, McVenes Rick, Stokes Ken

机构信息

Medtronic, Inc., 7000 Central Avenue NE, Minneapolis, MN 55432, USA.

出版信息

J Biomed Mater Res A. 2005 Oct 1;75(1):175-84. doi: 10.1002/jbm.a.30396.

Abstract

Polyethylene oxide (PEO) on polymer surfaces has been reported to reduce cellular adhesion, a very desirable property for cardiac pacing leads. A Shore 80A polyether polyurethane with up to 6% PEO surface-modifying end groups (SME) was evaluated for its chronic in vivo biostability. In a short-term (12 week) screening test, strained samples appeared to develop the same surface oxidation as unmodified polymer, but did not produce visible cracking > or =500x, prompting a longer-term study. By the time the longer-term study was initiated, most of the PEO SME had disappeared from the starting material's surface. After 1 year in vivo, surface oxidation, shallow surface cracking, and environmental stress cracking (ESC) developed on highly strained samples to the point of failure, so that there was no significant difference between the SME polymer and its control (the same polymer without SME). No further change was seen for up to 2 years of implantation. Unstrained PEO SME polymer developed shallow surface cracking, but no ESC up to 2 years of implantation. Thus, PEO SME slightly delayed, but did not stop biodegradation, and under unstrained conditions, has no adverse effect on biostability.

摘要

据报道,聚合物表面的聚环氧乙烷(PEO)可减少细胞黏附,这是心脏起搏导线非常理想的特性。对一种含有高达6% PEO表面改性端基(SME)的邵氏80A聚醚聚氨酯进行了长期体内生物稳定性评估。在一项短期(12周)筛选试验中,应变样品似乎与未改性聚合物发生了相同程度的表面氧化,但未产生大于或等于500倍的可见裂纹,因此开展了一项长期研究。在开始长期研究时,大部分PEO SME已从起始材料表面消失。体内植入1年后,高度应变的样品出现了表面氧化、浅表面裂纹和环境应力开裂(ESC),直至失效,因此SME聚合物与其对照物(不含SME的相同聚合物)之间没有显著差异。植入长达2年未见进一步变化。未应变的PEO SME聚合物出现了浅表面裂纹,但植入长达2年未出现ESC。因此,PEO SME略微延迟了生物降解,但并未阻止生物降解,并且在未应变条件下,对生物稳定性没有不利影响。

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