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含组织型纤溶酶原激活剂的聚氨酯表面的纤维蛋白溶解活性。

Tissue plasminogen activator-containing polyurethane surfaces for fibrinolytic activity.

机构信息

Macromolecules and Biointerface Laboratory, College of Chemistry, Chemical Engineering and Materials Science, Soochow University, Suzhou, People's Republic of China.

出版信息

Acta Biomater. 2011 May;7(5):1993-8. doi: 10.1016/j.actbio.2011.01.026. Epub 2011 Jan 21.

Abstract

With the aim of minimizing thrombus formation in blood-contacting devices, tissue plasminogen activator (t-PA)-containing polyurethane (PU) materials have been developed. Cationic PU surfaces were prepared by grafting poly(dimethylaminoethyl methacrylate) and quaternizing the tertiary amino groups with iodomethane or 1,6-diiodohexane or α,α'-dichloro-p-xylene. The surfaces were characterized by water contact angles and X-ray photoelectron spectroscopy. The materials (PU-CH(3)I, PU-I(CH(2))(6)I, PU-Cl) were treated with t-PA in Tris-buffered saline (pH 9.0) to give t-PA-loaded PU surfaces. The t-PA content of the surfaces was determined using radiolabeled t-PA. The quantities of t-PA taken up by the cationic surfaces were significantly greater than on the unmodified PU: approximately 14-fold greater for PU-Cl, 10-fold for PU-CH(3)I and 13-fold for PU-I(CH(2))(6)I. The activity of the bound t-PA, as measured by a plasma clotting-dissolution assay and a chromogenic substrate assay, was similar to that of normal, unbound t-PA. Release of t-PA from these materials in contact with plasma was measured using the labeled protein and was found to be the most rapid on the PU-CH(3)I material. This approach may have potential for the development of surfaces which can lyse clots that begin to form on them.

摘要

为了最大限度地减少与血液接触的装置中的血栓形成,已经开发了含有组织纤溶酶原激活剂(t-PA)的聚氨酯(PU)材料。通过接枝聚(二甲基氨基乙基甲基丙烯酸酯)并用碘甲烷或 1,6-二碘己烷或α,α'-二氯对二甲苯季铵化,制备了阳离子 PU 表面。通过水接触角和 X 射线光电子能谱对表面进行了表征。将这些材料(PU-CH(3)I、PU-I(CH(2))(6)I、PU-Cl)用 t-PA 在 Tris 缓冲盐水(pH 9.0)中处理,以得到负载 t-PA 的 PU 表面。使用放射性标记的 t-PA 测定表面的 t-PA 含量。阳离子表面吸收的 t-PA 量明显高于未改性的 PU:对于 PU-Cl,约增加 14 倍,对于 PU-CH(3)I 增加 10 倍,对于 PU-I(CH(2))(6)I 增加 13 倍。通过血浆凝块溶解测定和比色底物测定测量结合的 t-PA 的活性,与正常的未结合的 t-PA 相似。通过使用标记的蛋白质测量与血浆接触时这些材料中 t-PA 的释放,发现 PU-CH(3)I 材料的释放最快。这种方法可能有潜力开发能够溶解开始在其上形成的血栓的表面。

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