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用抗凝血酶-肝素复合物修饰用于血液接触的聚氨酯表面:用作连接子/间隔物的聚氧化乙烯分子量的影响。

Modification of polyurethane surface with an antithrombin-heparin complex for blood contact: influence of molecular weight of polyethylene oxide used as a linker/spacer.

机构信息

School of Biomedical Engineering, McMaster University, 1280 Main Street West, Hamilton, ON, Canada L8S 4K1.

出版信息

Langmuir. 2012 Jan 31;28(4):2099-106. doi: 10.1021/la203821g. Epub 2011 Dec 22.

Abstract

Polyurethane (PU) was modified using isocyanate chemistry to graft polyethylene oxide (PEO) of various molecular weights (range 300-4600). An antithrombin-heparin (ATH) covalent complex was subsequently attached to the free PEO chain ends, which had been functionalized with N-hydroxysuccinimide (NHS) groups. Surfaces were characterized by water contact angle and X-ray photoelectron spectroscopy (XPS) to confirm the modifications. Adsorption of fibrinogen from buffer was found to decrease by ~80% for the PEO-modified surfaces compared to the unmodified PU. The surfaces with ATH attached to the distal chain end of the grafted PEO were equally protein resistant, and when the data were normalized to the ATH surface density, PEO in the lower MW range showed greater protein resistance. Western blots of proteins eluted from the surfaces after plasma contact confirmed these trends. The uptake of ATH on the PEO-modified surfaces was greatest for the PEO of lower MW (300 and 600), and antithrombin binding from plasma (an indicator of heparin anticoagulant activity) was highest for these same surfaces. The PEO-ATH- and PEO-modified surfaces also showed low platelet adhesion from flowing whole blood. It is concluded that for the PEO-ATH surfaces, PEO in the low MW range, specifically MW 600, may be optimal for achieving an appropriate balance between resistance to nonspecific protein adsorption and the ability to take up ATH and bind antithrombin in subsequent blood contact.

摘要

聚氨基甲酸乙酯(PU)经异氰酸酯化学修饰,接枝不同分子量的聚氧化乙烯(PEO)(范围 300-4600)。随后,将肝素抗凝血酶(ATH)共价复合物附着到经 N-羟基琥珀酰亚胺(NHS)基团官能化的游离 PEO 链末端。通过水接触角和 X 射线光电子能谱(XPS)对表面进行特性分析,以确认修饰。与未修饰的 PU 相比,PEO 修饰表面吸附缓冲液中的纤维蛋白原减少了约 80%。与附着在接枝 PEO 远端链末端的 ATH 相比,这些表面同样具有抗蛋白性,并且当数据归一化为 ATH 表面密度时,低分子量范围的 PEO 显示出更强的抗蛋白性。从等离子体接触后的表面洗脱的蛋白质的 Western 印迹证实了这些趋势。PEO 修饰表面对低分子量(300 和 600)PEO 的 ATH 摄取量最大,并且这些相同表面的血浆中抗凝血酶结合(肝素抗凝活性的指标)最高。PEO-ATH-和 PEO 修饰表面也显示出从流动全血中血小板黏附率低。结论是,对于 PEO-ATH 表面,低分子量的 PEO(特别是分子量 600)可能是在抵抗非特异性蛋白质吸附的能力和在随后的血液接触中摄取 ATH 和结合抗凝血酶之间取得适当平衡的最佳选择。

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