首页> 外文期刊>Biomacromolecules >Synthesis, Characterization, and Paditaxel Release from a Biodegradable, Elastomeric, Poly(ester urethane)urea Bearing Phosphorylcholine Groups for Reduced Thrombogenicity
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Synthesis, Characterization, and Paditaxel Release from a Biodegradable, Elastomeric, Poly(ester urethane)urea Bearing Phosphorylcholine Groups for Reduced Thrombogenicity

机译:从可降解的,具有弹性的,含磷酸胆碱基团的可生物降解的,弹性体,聚(酯氨基甲酸酯)脲的合成,表征和Paditaxel释放以降低血栓形成

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摘要

Biodegradable polymers with high elasticity, low thrombogenicity, and drug loading capacity continue to be pursued for vascular engineering applications, including vascular grafts and stents. A biodegradable elastomeric polyurethane was designed as a candidate material for use as a drug-eluting stent coating, such that it was nonthrombogenic and could provide antiproliferative drug release to inhibit smooth muscle cell proliferation. A phosphorylcholine containing poly(ester urethane) urea (PEUU-PC) was synthesized by-grafting aminated phosphorylcholine onto backbone carboxyl groups of a polyurethane (PEUU-COOH) synthesized from a soft segment blend of polycaprolactone and dimethylolpropionic acid, a hard segment of diisocyanatobutane and a putrescine chain extender. Poly(ester urethane) urea (PEUU) from a soft segment of polycaprolactone alone was employed as a control material. All of the synthesized polyurethanes showed high distensibility (>600%) and tensile strengths in the 20-35 MPa range. PEUU-PC experienced greater degradation than PEUU or PEUU-COOH in either a saline or lipase enzyme solution. PEUU-PC also exhibited markedly inhibited ovine blood platelet deposition compared with PEUU-COOH and PEUU. Paclitaxel loaded in all of the polymers during solvent casting continued to release for 5 d after a burst release in a 10% ethanol/PBS solution, which was utilized to increase the solubility of the releasate. Rat smooth muscle cell proliferation was significantly inhibited in 1 wk cell culture when releasate from the paclitaxel-loaded films was present. Based on these results, the synthesized PEUU-PC has promising functionality for use as a nonthrombogenic, drug eluting coating on metallic vascular stents and grafts.
机译:具有高弹性,低血栓形成性和载药量的可生物降解的聚合物继续用于包括血管移植物和支架在内的血管工程应用。设计了一种可生物降解的弹性体聚氨酯作为用作药物洗脱支架涂层的候选材料,这样它就不会血栓形成,并且可以提供抗增殖药物释放来抑制平滑肌细胞增殖。通过将胺化的磷酸胆碱接枝到由聚己内酯和二羟甲基丙酸的软链段共混物(二异氰酸根合丁烷的硬链段)合成的聚氨酯(PEUU-COOH)的主链羧基上,合成了一种含磷酸酯胆碱的聚(酯氨基甲酸酯)脲(PEUU-PC)。和腐胺扩链剂。仅将聚己内酯的软链段的聚(酯氨基甲酸酯)脲(PEUU)用作对照材料。所有合成的聚氨酯均显示出高分散性(> 600%)和20-35 MPa范围内的拉伸强度。在盐水或脂肪酶溶液中,PEUU-PC的降解均比PEUU或PEUU-COOH大。与PEUU-COOH和PEUU相比,PEUU-PC还显示出明显抑制的绵羊血小板沉积。在溶剂流延过程中加载到所有聚合物中的紫杉醇在10%乙醇/ PBS溶液中突然释放后继续释放5天,这被用来增加释放物的溶解度。当载有紫杉醇的薄膜释放时,大鼠的平滑肌细胞增殖在1周的细胞培养中被显着抑制。基于这些结果,合成的PEUU-PC具有有希望的功能,可用作金属血管支架和移植物上的非血栓性药物洗脱涂层。

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