首页> 外文期刊>International Journal of Polymeric Materials >Grafting of sulfamethoxazole on acrylic acid-vinyl methyl ketone copolymer using the schiff base reaction-application as a drug delivery system
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Grafting of sulfamethoxazole on acrylic acid-vinyl methyl ketone copolymer using the schiff base reaction-application as a drug delivery system

机译:使用Schiff基碱反应应用作为药物递送系统的亚克酸 - 乙烯基甲基酮共聚物覆盖亚磺酰胺 - 乙烯基甲基酮共聚物

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摘要

A series of poly(acrylic acid-co-methylvinylketone-graft-sulfamethoxazole)(AVMDS) species was synthesized for drug carrier applications. The synthesis involved two steps: copolymerization of acrylic acid(AA) with methyl vinyl ketone(MVK) through the free radical route and subsequent grafting of the sulfamethoxazole (SMX) onto the copolymer via the Schiff base reaction of the primary amine of SMX with the carbonyl groups of the MVK units. The structures and properties of the materials were characterized by nuclear magnetic resonance(NMR), X-ray diffraction(XRD), differential scanning calorimetry(DSC), and scanning electronic microscopy (SEM). An in-vitro cytotoxicity test of the drug-carrier systems via MTT assay revealed no significant cytotoxic effect at concentrations up to 100 mu g center dot ml(-1). The dynamic release of SMX from these systems through a retro-imidation reaction (inverse Schiff base reaction) was investigated in depth, where the diffusion through the polymer matrix, the enhancement of the water solubility of SMX, the influence of the initial drug concentration, the pH of the medium, and the effect of the degree of swelling of the polymer matrix on the release dynamics were evaluated. The AVMGS4 and AVMGS1 drug carrier systems containing 3.58 and 1.18 wt% of SMX were the best performing systems.
机译:为药物载体应用合成了一系列聚(丙烯酸 - 共聚甲基丙酮 - 移植物 - 磺胺甲氧唑)(AVMDS)物种。合成涉及两步:通过自由基途径将丙烯酸(AA)与甲基乙烯基酮(MVK)共聚,并随后通过SMX伯胺的粒碱反应将磺胺甲恶唑(SMX)接枝到共聚物上MVK单元的羰基。材料的结构和性质的特征在于核磁共振(NMR),X射线衍射(XRD),差示扫描量热法(DSC)和扫描电子显微镜(SEM)。通过MTT测定的药物 - 载体系统的体外细胞毒性试验显示在浓度上没有显着的细胞毒性作用,高达100μg中心点M1(-1)。深入研究了通过复古 - 酰亚胺反应(逆席夫基反应)从这些系统的动态释放,其中通过聚合物基质的扩散,SMX的水溶性的增强,初始药物浓度的影响,评价培养基的pH和聚合物基质溶胀程度对释放动力学的影响。 AVMGS4和AVMGS1药物载体系统含有3.58和1.18wt%的SMX是最佳性能的系统。

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