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首页> 外文期刊>Dental materials >Effects of solubilizing surfactants and loading of antiviral antimicrobial, and antifungal drugs on their release rates from ethylene vinyl acetate copolymer
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Effects of solubilizing surfactants and loading of antiviral antimicrobial, and antifungal drugs on their release rates from ethylene vinyl acetate copolymer

机译:增溶表面活性剂和抗病毒抗菌剂和抗真菌药的添加对其从乙烯乙酸乙烯酯共聚物中释放速率的影响

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Objectives. This study investigates the effects of surfactants and drug loading on the drug release rate from ethylene vinyl acetate (EVA) copolymer. The release rate of nystatin from EVA was studied with addition of non-ionic surfactants Tween 60 and Cremophor RH 40. In addition, the effect of increasing drug load on the release rates of nystatin, chlorhexidine diacetate and acyclovir is also presented. Method. Polymer casting solutions were prepared by stirring EVA copolymer and nystatin (2.5wt.%) in dichloromethane. Nystatin and surfactants were added in ratios of (1:1), (1:2) and (1:3). Drug loading was studied with 2.5, 5.0, 7.5, and 10.0wt.% proportions of nystatin, chlorhexidine diacetate and acyclovir incorporated into a separate polymer. Three drug loaded polymer square films (3 cm x 3 cm x 0.08 cm) were cut from dry films to follow the kinetics of drug release at 37℃. Ten milliliters of either distilled water or PBS was used as the extracting medium that was replaced daily. PBS was used for nystatin release with addition of surfactants and water was used for the study on drug loading and surfactant release. The rate of drug release was measured by UV-spectrophotometer. The amount of surfactant released was determined by HPLC. Results. The release of nystatin was low in PBS and its release rate increased with the addition of surfactants. Also, increasing surfactant concentrations resulted in increased drug release rates. The release rates of chlorhexidine diacetate (p < 0.0001), acyclovir (p < 0.0003) and nystatin (p < 0.0017) linearly increased with increasing drug loads. The amount of surfactants released was above the CMC. Significance. This study demonstrates that the three therapeutic agents show a sustained rate of drug release from EVA copolymer over extended periods of time. Nystatin release in PBS is low owing to its poor solubility. Its release rate is enhanced by addition of surfactants and increasing the drug load as well.
机译:目标。这项研究调查了表面活性剂和载药量对乙烯乙酸乙烯酯(EVA)共聚物药物释放速率的影响。在添加非离子表面活性剂Tween 60和Cremophor RH 40的情况下,研究了制霉菌素从EVA的释放速率。此外,还提出了增加载药量对制霉菌素,双氧氯己定和阿昔洛韦的释放速率的影响。方法。通过在二氯甲烷中搅拌EVA共聚物和制霉菌素(2.5wt。%)来制备聚合物浇铸溶液。制霉菌素和表面活性剂的比例为(1:1),(1:2)和(1:3)。用2.5%,5.0%,7.5%和10.0wt。%比例的制霉菌素,洗必泰双乙酸酯和无环鸟苷掺入单独的聚合物中研究了药物的负载。从干膜上切下三片载药的聚合物正方形薄膜(3 cm x 3 cm x 0.08 cm),以追踪在37℃释放药物的动力学。每天更换十毫升的蒸馏水或PBS作为提取介质。 PBS用于制霉菌素的释放,同时添加表面活性剂,而水用于研究载药量和表面活性剂的释放。药物释放速率通过紫外分光光度计测量。通过HPLC测定释放的表面活性剂的量。结果。制霉菌素在PBS中的释放较低,并且其释放速率随着表面活性剂的添加而增加。同样,增加表面活性剂浓度导致增加的药物释放速率。随着药物负荷的增加,双乙酸洗必泰(p <0.0001),阿昔洛韦(p <0.0003)和制霉菌素(p <0.0017)的释放速率线性增加。释放的表面活性剂的量高于CMC。意义。这项研究表明,三种治疗剂在较长的时间内显示出从EVA共聚物中持续释放药物的速率。由于其不良的溶解性,制霉菌素在PBS中的释放较低。通过添加表面活性剂并增加药物负荷来提高其释放速率。

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