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Development and hemocompatibility testing of nitric oxide releasing polymers using a rabbit model of thrombogenicity

机译:使用兔血栓形成模型开发和释放一氧化氮聚合物的血液相容性测试

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摘要

Hemocompatibility is the goal for any biomaterial contained in extracorporeal life supporting (ECLS) medical devices. The hallmarks for hemocompatibility include nonthrombogenicity, platelet preservation and maintained platelet function. Both in vitro and in vivo assays testing for compatibility of the blood/biomaterial interface have been used over the last several decades to ascertain if the biomaterial used in medical tubing and devices will require systemic anticoagulation for viability. Over the last 50 years systemic anticoagulation with heparin has been the gold standard in maintaining effective ECLS. However, the biomaterial that maintains effective ECLS without the use of any systemic anticoagulant has remained elusive. In this review, the in vivo 4-h rabbit thrombogenicity model genesis will be described with emphasis on biomaterials that may require no systemic anticoagulation for ECLS longevity. These novel biomaterials may improve extracorporeal circulation (ECC) hemocompatibility by preserving near resting physiology of the major blood components, the platelets and monocytes. The rabbit ECC model provides a complete assessment of biomaterial interactions with the intrinsic coagulation players, the circulating platelet and monocytes. This total picture of blood/biomaterial interaction suggests that this rabbit thrombogenicity model could provide a standardization for biomaterial hemocompatibility testing.
机译:血液相容性是体外生命支持(ECLS)医疗设备中包含的任何生物材料的目标。血液相容性的标志包括非血栓形成性,血小板保存和维持血小板功能。在过去的几十年中,已经使用体外和体内试验来测试血液/生物材料界面的相容性,以确定用于医疗管道和设备的生物材料是否需要系统性抗凝以提高生存能力。在过去的50年中,肝素的全身抗凝治疗一直是维持有效ECLS的金标准。然而,在不使用任何全身性抗凝剂的情况下维持有效ECLS的生物材料仍然难以捉摸。在这篇综述中,将描述体内4-h兔血栓形成模型的发生,重点是对于ECLS长寿可能不需要全身性抗凝的生物材料。这些新型生物材料可以通过保留主要血液成分,血小板和单核细胞的近乎静止的生理状态来改善体外循环(ECC)血液相容性。兔ECC模型提供了对生物材料与固有凝血因子,循环血小板和单核细胞相互作用的完整评估。血液/生物材料相互作用的总体情况表明,这种兔血栓形成模型可以为生物材料血液相容性测试提供标准化。

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