涂层
材料科学
血栓形成
肝素
血栓调节蛋白
聚四氟乙烯
生物医学工程
血小板
纳米技术
外科
复合材料
医学
血栓形成
凝血酶
内科学
作者
Hyun Ok Ham,Carolyn A. Haller,Guowei Su,Erbin Dai,Madhukar S. Patel,David R. Liu,Jian Liu,Elliot L. Chaikof
出处
期刊:Biomaterials
[Elsevier]
日期:2021-07-09
卷期号:276: 121011-121011
被引量:10
标识
DOI:10.1016/j.biomaterials.2021.121011
摘要
Despite the potential of anti-thrombogenic coatings, including heparinized surfaces, to improve the performance of blood-contacting devices, the inevitable deterioration of bioactivity remains an important factor in device failure and related thrombotic complications. As a consequence, the ability to restore the bioactivity of a surface coating after implantation of a blood-contacting device provides a potentially important strategy to enhance its clinical performance. Here, we report the regeneration of a multicomponent anti-thrombogenic coating through use of an evolved sortase A to mediate reversible transpeptidation. Both recombinant thrombomodulin and a chemoenzymatically synthesized ultra-low molecular weight heparin were repeatedly and selectively immobilized or removed in a sequential, alternating, or simultaneous manner. The generation of activated protein C (aPC) and inhibition of activated factor X (FXa) was consistent with the molecular composition of the surface. The fabrication of a rechargeable anti-thrombogenic surface was demonstrated on an expanded polytetrafluoroethylene (ePTFE) vascular graft with reconstitution of the surface bound coating 4 weeks after in vivo implantation in a rat model.
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