涂层支架:局部药理学。

V K Raman, E R Edelman
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引用次数: 0

摘要

尽管急性血管灌注恢复良好,但冠状动脉支架植入术仍受到3-10天内亚急性血栓形成和干预后6个月内膜增生导致再狭窄的限制。为了预防这些后遗症,已经使用了多种药物治疗方法。减少血栓形成的药物方案有可能产生严重的毒性,而且迄今为止没有任何方案在临床上显示可以减少再狭窄的发生率。通过涂有固定药物或涂有药物释放聚合物基质的支架进行局部药物递送,可以在靶组织内提供局部治疗药物效果,而不会因全身给药而产生严重的副作用。然而,在这种治疗方式的前景实现之前,需要更详细地了解局部药理学对药物活性的影响。药物装置参数(如支架表面积和药物附着方式)和药物组织参数(包括药物在组织中的溶解度和与组织的非特异性结合)以复杂的方式相互作用,以确定局部组织药物剂量、分布,从而确定效果。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Coated stents: local pharmacology.

Despite excellent restoration of acute vessel perfusion, coronary stenting has been limited by subacute thrombosis within 3-10 days and by neointimal proliferation leading to restenosis by 6 months post-intervention. A variety of pharmacotherapeutics have been utilized in an attempt to prevent these sequelae. Drug regimens that reduce thrombosis have the potential for serious toxicities, and no regimen to date has been shown clinically to reduce the incidence of restenosis. Local drug delivery via stents coated with immobilized drug or coated with a drug-releasing polymer matrix offers the possibility of focal therapeutic drug effect within target tissues without serious side-effects arising from systemic drug administration. Before the promise of this treatment modality is realized, however, a more detailed understanding is needed of the local pharmacologic influences on drug activity. Drug-device parameters, such as stent surface area and mode of drug attachment, and drug-tissue parameters, including drug solubility in and non-specific binding to tissues, interact in a complex manner to determine local tissue drug dose, distribution and, consequently, effect.

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