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载eptifibatide 可降解纳米粒子对聚氨酯的表面修饰降低血液凝固风险。

Surface modification of polyurethane with eptifibatide-loaded degradable nanoparticles reducing risk of blood coagulation.

机构信息

AGH University of Science and Technology, Faculty of Materials Science and Ceramics, Al. Mickiewicza 30, 30-059 Kraków, Poland.

Institute of Metallurgy and Materials Science, Polish Academy of Sciences, 25 Reymonta st., 30-059 Cracow, Poland.

出版信息

Colloids Surf B Biointerfaces. 2021 May;201:111624. doi: 10.1016/j.colsurfb.2021.111624. Epub 2021 Feb 13.

Abstract

The main purpose of the work was to develop a drug releasing coatings on the surface of medical devices exposed to blood flow, what should enable effective inhibition of blood coagulation process. As a part of the work, the process of encapsulating the anticoagulant drug eptifibatide (EPT) in poly(DL-lactic-co-glycolic acid) (PLGA) nanoparticles was developed. EPT encapsulation efficiency was 29.1 ± 2.1%, while the EPT loading percentage in the nanoparticles was 4.2 ± 0.3%. The PLGA nanoparticles were suspended in a polyanion solution (hyaluronic acid (HA)) and deposited on the surface-treated thermoplastic polyurethane (TPU) by a layer-by-layer method. As a polycation poly-L-lysine (PLL) was used. The influence of released EPT on the activation of the coagulation system was analyzed using dynamic blood tester. Performed experiments show an effective delivery of the drug to the bloodstream and low risk of platelets (membrane receptor) activation. The dynamic blood test process, including its physical phenomenon, was described using numerical methods, i.e. a finite volume cone-and-plate test model as well as non-Newtonian blood models. The values of shear stress and blood flow velocity under the fast-rotating cone were computed applying boundary conditions of cylinder wall imitating blood-nanomaterial interaction. Implementing boundary conditions as initial shear stress values of bottom cylinder wall resulted in the increase of shear stress in blood under rotating cone. The developed system combining drug eluting polymeric nanoparticles with the polyelectrolyte "layer-by-layer" coating can be easily introduced to medical implants of various shape, with the advantages of resorbable drug carriers allowing for local and controllable delivery of anti-thrombogenic drugs.

摘要

这项工作的主要目的是开发一种能够在暴露于血流的医疗器械表面释放药物的涂层,从而有效抑制血液凝固过程。作为这项工作的一部分,我们开发了将抗凝药物依替巴肽(EPT)包封在聚(DL-丙交酯-共-乙交酯)(PLGA)纳米粒子中的方法。EPT 的包封效率为 29.1 ± 2.1%,而纳米粒子中 EPT 的载药量为 4.2 ± 0.3%。PLGA 纳米粒子悬浮在聚阴离子溶液(透明质酸(HA))中,并通过层层沉积法沉积在经过表面处理的热塑性聚氨酯(TPU)上。使用聚阳离子聚-L-赖氨酸(PLL)作为聚电解质。通过动态血液测试仪分析释放的 EPT 对凝血系统激活的影响。实验表明,药物能够有效递送到血液中,且血小板(膜受体)激活的风险较低。使用数值方法描述了动态血液测试过程及其物理现象,即有限体积的圆锥板测试模型以及非牛顿血液模型。应用模拟血液-纳米材料相互作用的圆柱壁边界条件计算了快速旋转圆锥下的剪切应力和血流速度值。该系统将载药聚合物纳米粒子与聚电解质“层层”涂层相结合,可以很容易地引入到各种形状的医疗植入物中,具有可吸收药物载体的优点,允许局部和可控地输送抗血栓药物。

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