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Dual-Layer Coated Drug-Eluting Stents with Improved Degradation Morphology and Controlled Drug Release

机译:双层涂层药物洗脱支架,具有改善的降解形态和控制药物释放

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摘要

Drug-eluting stents (DESs) are used to treat cardiovascular diseases such as atherosclerosis. The anti-proliferative drug released from the DES suppress the proliferation of smooth muscle cells and reduced in-stent restenosis. However, a burst release of the drug in the early stages and degradation morphology of the polymer coating represent major disadvantages, which might increase the incidence of in-stent restenosis and/or thrombosis under in vivo clinical studies. To solve these problems, in this study, a double-layer coating system composed of poly(lactide) (PLLA) bottom layer and poly(lactide-co-glycolide) (PLGA) top layer are used for the fabrication of DES. PLLA bottom layer was firstly coated on the metal surface followed by oxygen ion beam treatment. It was found that increasing the ion beam exposure time, increased the roughness of PLLA surface with a nanoscale pocket (or hole)-like structure. The top layer coating represented a mixture of PLGA and paclitaxel (PTX) with 5, 10, and 20% PTX contents. The coating was performed through ultrasonic spray technique, and the morphology showed not only a smooth and uniform surface but also no irregularities were observed at zero day. The drug release and degradation morphology for single-layer (PLGA/PTX) and double-layer (PLLA/PLGA/PTX) coatings were compared. The drug release from the double-layer stainless steel (SS) group showed a slower and controlled drug release for all PTX content samples as compared to single-layer SS group. Moreover, the degradation morphology of double-layer SS group presented a smoother and uniform surface after 12 weeks of degradation under physiological conditions. Therefore, an oxygen ion beam technique with double-layer coating system could effectively control the drug release, i.e., prevent initial burst drug release, and improve the degradation morphology of biodegradable polymer-based DESs.
机译:药物洗脱支架(DESS)用于治疗诸如动脉粥样硬化的心血管疾病。从DES中释放的抗增殖药物抑制了平滑肌细胞的增殖,降低了支架内再狭窄。然而,在高分子涂料的早期阶段和降解形态中药物的突发释放是主要缺点,这可能会增加体内临床研究中的支架内再狭窄和/或血栓形成的主要缺点。为了解决这些问题,在该研究中,由聚(丙交酯)(PLLA)底层和聚(丙交酯 - 共乙酰化)(PLGA)顶层组成的双层涂层系统用于制造DES。首先涂覆在金属表面上的PLLA底层,然后氧气离子束处理。发现增加离子束曝光时间,增加了用纳米级口袋(或孔)的结构的PLLA表面的粗糙度。顶层涂层表示PLGA和紫杉醇(PTX)的混合物,其中5,10和20%PTX含量。通过超声波喷射技术进行涂层,并且形态不仅表现出光滑且均匀的表面,而且在零天内没有观察到不规则性。比较了单层(PLGA / PTX)和双层(PLLA / PLGA / PTX)涂层的药物释放和降解形态。与单层SS组相比,双层不锈钢(SS)组中的药物释放为所有PTX含量样品显示出较慢的和控制的药物释放。此外,在生理条件下在降解12周后,双层SS组的降解形态呈现更平滑和均匀的表面。因此,具有双层涂层系统的氧离子束技术可以有效地控制药物释放,即防止初始爆破药物释放,并改善生物降解的聚合物的DES的降解形态。

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