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The effect of a polyurethane coating incorporating both a thrombin inhibitor and nitric oxide on hemocompatibility in extracorporeal circulation

机译:凝血酶抑制剂和一氧化氮的聚氨酯涂料对体外循环血液相容性的影响

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摘要

Nitric oxide (NO) releasing (NORel) materials have been extensively investigated to create localized increases in NO concentration by the proton driven diazeniumdiolate-containing polymer coatings and demonstrated to improve extracorporeal circulation (ECC) hemocompatibility. In this work, the NORel polymeric coating composed of a diazeniumdiolated dibutylhexanediamine (DBHD-N2O2)-containing hydrophobic Elast-eon (E2As) polyurethane was combined with a direct thrombin inhibitor, argatroban (AG), and evaluated in a 4 h rabbit thrombogenicity model without systemic anticoagulation. In addition, the immobilizing of argatroban to E2As polymer was achieved by either a polyethylene glycol-containing (PEGDI) or hexane methylene (HMDI) diisocyanate linker. The combined polymer film was coated on the inner walls of ECC circuits to yield significantly reduced ECC thrombus formation compared to argatroban alone ECC control after 4 h blood exposure (0.6 ± 0.1 AG/HMDI/NORel vs 1.7 ± 0.2 cm2 AG/HMDI control). Platelet count (2.8 ± 0.3 AG/HMDI/NORel vs 1.9 ± 0.1 × 108/ml AG/HMDI control) and plasma fibrinogen levels were preserved after 4 h blood exposure with both the NORel/argatroban combination and the AG/HMDI control group compared to baseline. Platelet function as measured by aggregometry remained near normal in both the AG/HMDI/NORel (63 ± 5%) and AG/HMDI control (58 ± 7%) groups after 3 h compared to baseline (77 ± 1%). Platelet P-selectin mean fluorescence intensity (MFI) as measured by flow cytometry also remained near baseline levels after 4 h on ECC to ex vivo collagen stimulation (16 ± 3 AG/HMDI/NORel vs 11 ± 2 MFI baseline). These results suggest that the combined AG/HMDI/NORel polymer coating preserves platelets in blood exposure to ECCs to a better degree than AG/PEGDI/NORel, NORel alone or AG alone. These combined antithrombin, NO-mediated antiplatelet effects were shown to improve thromboresistance of the AG/HMDI/NORel polymer-coated ECCs and move potential nonthrombogenic polymers closer to mimicking vascular endothelium.
机译:已经广泛研究了释放一氧化氮(NO)的材料(NORel),以通过质子驱动的含二醇二氮烯二酸酯的聚合物涂层使NO浓度局部升高,并证明可改善体外循环(ECC)的血液相容性。在这项工作中,将由含重氮二醇二丁基己二胺(DBHD-N2O2)的疏水性Elast-eon (E2As)聚氨酯组成的NORel聚合物涂料与直接凝血酶抑制剂,阿加曲班(AG)和在没有全身性抗凝的4小时兔血栓形成模型中进行了评估。此外,通过含聚乙二醇的(PEGDI)或己烷亚甲基(HMDI)的二异氰酸酯连接基将Argatroban固定在E2As聚合物上。血液暴露4 h后,与单独使用argatroban的ECC控制相比,将合并的聚合物薄膜涂覆在ECC电路的内壁上,从而显着减少了ECC血栓的形成(0.6±0.1 AG / HMDI / NORel与1.7±0.2 cm 2 < / sup> AG / HMDI控件)。 NORel / argatroban组合暴露4 h后,血小板计数(2.8±0.3 AG / HMDI / NORel与1.9±0.1×10 8 / ml AG / HMDI对照)和血浆纤维蛋白原水平得以保持并将AG / HMDI对照组与基线进行比较。与基线时(77±1%)相比,在3小时后,AG / HMDI / NORel(63±5%)和AG / HMDI对照(58±7%)组中通过凝集测定法测得的血小板功能仍接近正常。通过流式细胞术测量的血小板P-选择素平均荧光强度(MFI)在ECC对离体胶原蛋白刺激后4小时后也保持在基线水平附近(16±3 AG / HMDI / NORel与11±2 MFI基线)。这些结果表明,组合的AG / HMDI / NORel聚合物涂层在血液中暴露于ECC的血小板比AG / PEGDI / NORel,单独的NORel或单独的AG更好。这些组合的抗凝血酶,NO介导的抗血小板作用已显示可改善AG / HMDI / NORel聚合物涂层的ECC的抗血栓性,并使潜在的非血栓形成性聚合物更接近于模仿血管内皮。

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