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Modification of polyurethane with polyethylene glycol-corn trypsin inhibitor for inhibition of factor XIIa in blood contact

机译:用聚乙二醇-玉米胰蛋白酶抑制剂修饰聚氨酯以抑制血液接触中的因子XIIa

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In previous work using gold as a model substrate, we showed that modification of surfaces with poly(ethylene glycol) (PEG) and corn trypsin inhibitor (CTI) rendered them protein resistant and inhibitory against activated factor XII. Sequential attachment of PEG followed by CTI gave superior performance compared to direct attachment of a preformed PEG-CTI conjugate. In the present work, a sequential method was used to attach PEG and CTI to a polyurethane (PU) substrate to develop a material with applicability for blood-contacting medical devices. Controls included surfaces modified only with PEG and only with CTI. Surfaces were characterized by water contact angle and X-ray photoelectron spectroscopy. The surface density of CTI was in the range of a monolayer and was higher on the PU substrate than on gold reported previously. Biointeractions were investigated by measuring fibrinogen adsorption from buffer and plasma, factor XIIa inhibition and plasma clotting time. Both the PU-PEG surfaces and the PU-PEG-CTI surfaces showed low fibrinogen adsorption from buffer and plasma, indicating that PEG retained its protein resistance when conjugated to CTI. Although the CTI density was lower on PU-PEG-CTI than on PU modified only with CTI, PU-PEG-CTI exhibited greater factor XIIa inhibition and a longer plasma clotting time, suggesting that PEG facilitates the interaction of CTI with factor XIIa. Thus sequential attachment of PEG and CTI may be a useful approach to improve the thromboresistance of PU surfaces.
机译:在以前使用金作为模型底物的工作中,我们表明用聚乙二醇(PEG)和玉米胰蛋白酶抑制剂(CTI)修饰表面使其具有蛋白质抗性和抑制活化因子XII的能力。与直接附着的PEG-CTI共轭物相比,依次附着PEG和CTI产生了优越的性能。在当前的工作中,使用了一种顺序方法将PEG和CTI连接到聚氨酯(PU)基材上,以开发一种适用于血液接触医疗设备的材料。对照包括仅用PEG和仅用CTI修饰的表面。通过水接触角和X射线光电子能谱表征表面。 CTI的表面密度在单层范围内,在PU基材上比以前报道的在金上更高。通过测量纤维蛋白原从缓冲液和血浆中的吸附,因子XIIa抑制和血浆凝结时间来研究生物相互作用。 PU-PEG表面和PU-PEG-CTI表面均显示出较低的纤维蛋白原从缓冲液和血浆中的吸附,表明PEG与CTI偶联时保留了其蛋白抗性。尽管PU-PEG-CTI的CTI密度比仅用CTI改性的PU低,但PU-PEG-CTI表现出更大的XIIa抑制因子和更长的血浆凝结时间,表明PEG促进CTI与XIIa因子的相互作用。因此,PEG和CTI的顺序连接可能是提高PU表面抗血栓性的有用方法。

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