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神经血管支架的表面改性:从实验室到临床。

Surface modification of neurovascular stents: from bench to patient.

机构信息

New England Center for Stroke Research, Department of Radiology, University of Massachusetts Chan Medical School, Worcester, Massachusetts, USA.

Neurosurgery, Icahn School of Medicine at Mount Sinai, New York, New York, USA.

出版信息

J Neurointerv Surg. 2024 Aug 14;16(9):908-913. doi: 10.1136/jnis-2023-020620.

Abstract

Flow-diverting stents (FDs) for the treatment of cerebrovascular aneurysms are revolutionary. However, these devices require systemic dual antiplatelet therapy (DAPT) to reduce thromboembolic complications. Given the risk of ischemic complications as well as morbidity and contraindications associated with DAPT, demonstrating safety and efficacy for FDs either without DAPT or reducing the duration of DAPT is a priority. The former may be achieved by surface modifications that decrease device thrombogenicity, and the latter by using coatings that expedite endothelial growth. Biomimetics, commonly achieved by grafting hydrophilic and non-interacting polymers to surfaces, can mask the device surface with nature-derived coatings from circulating factors that normally activate coagulation and inflammation. One strategy is to mimic the surfaces of innocuous circulatory system components. Phosphorylcholine and glycan coatings are naturally inspired and present on the surface of all eukaryotic cell membranes. Another strategy involves linking synthetic biocompatible polymer brushes to the surface of a device that disrupts normal interaction with circulating proteins and cells. Finally, drug immobilization can also impart antithrombotic effects that counteract normal foreign body reactions in the circulatory system without systemic effects. Heparin coatings have been explored since the 1960s and used on a variety of blood contacting surfaces. This concept is now being explored for neurovascular devices. Coatings that improve endothelialization are not as clinically mature as anti-thrombogenic coatings. Coronary stents have used an anti-CD34 antibody coating to capture circulating endothelial progenitor cells on the surface, potentially accelerating endothelial integration. Similarly, coatings with CD31 analogs are being explored for neurovascular implants.

摘要

血流导向装置(FDs)在治疗脑血管动脉瘤方面是革命性的。然而,这些设备需要全身性双联抗血小板治疗(DAPT)来降低血栓栓塞并发症的风险。鉴于缺血性并发症的风险,以及 DAPT 相关的发病率和禁忌症,证明 FDs 无需 DAPT 或减少 DAPT 持续时间的安全性和有效性是当务之急。前者可以通过降低器械血栓形成性的表面修饰来实现,后者可以通过使用促进内皮细胞生长的涂层来实现。仿生学通常通过将亲水性和非相互作用的聚合物接枝到表面上来实现,可以用来自循环因子的天然衍生涂层来掩盖器械表面,这些循环因子通常会激活凝血和炎症。一种策略是模拟无害的循环系统组件的表面。磷酸胆碱和聚糖涂层是天然存在的,存在于所有真核细胞膜的表面。另一种策略涉及将合成生物相容性聚合物刷连接到器械表面,从而破坏与循环蛋白和细胞的正常相互作用。最后,药物固定化也可以赋予抗血栓作用,抵消循环系统中正常异物反应,而不会产生全身效应。肝素涂层自 20 世纪 60 年代以来就一直在探索,并用于各种与血液接触的表面。现在正在探索将其用于神经血管设备。促进内皮化的涂层不如抗血栓形成的涂层在临床上成熟。冠状动脉支架已经使用抗 CD34 抗体涂层来捕获表面上的循环内皮祖细胞,从而可能加速内皮整合。类似地,正在探索用于神经血管植入物的具有 CD31 类似物的涂层。

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