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用于口腔环境中递送洗必泰和阿昔洛韦药物的聚(乙烯 - 共 - 醋酸乙烯酯)共聚物基质:药物组合、共聚物组成和包衣对药物释放速率的影响

Poly(ethylene-co-vinyl acetate) copolymer matrix for delivery of chlorhexidine and acyclovir drugs for use in the oral environment: effect of drug combination, copolymer composition and coating on the drug release rate.

作者信息

Tallury Padmavathy, Alimohammadi Nazila, Kalachandra Sid

机构信息

Center for Oral and Systemic Diseases, Department of Periodontology, School of Dentistry, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599-7455, USA.

出版信息

Dent Mater. 2007 Apr;23(4):404-9. doi: 10.1016/j.dental.2006.02.011. Epub 2006 Mar 23.

Abstract

OBJECTIVES

This study utilizes a bio-compatible ethylene vinyl acetate (EVA) copolymer to deliver drugs at therapeutic levels over extended periods of time. The release rate of an anti-fungal and an anti-microbial drug namely acyclovir (ACY) and chlorhexidine diacetate (CDA) from EVA was investigated individually and as a mixture. The effect of drug combination, the composition of the copolymer and the coating of the matrix with a different polymer on the rate of drug release are presented.

METHOD

Polymer casting solutions were prepared by homogeneously dissolving EVA copolymer and the drugs in the ratio (40:1) in dichloromethane. The drugs ACY and CDA were used individually as well as in three different weight ratios maintaining the total drug concentration in the polymer at 2.5%. Different concentrations of vinyl acetate (VA) 28, 32 and 40% in the EVA matrix were used to study the release of either ACY or CDA alone while 40% VA was used for the release study of the individual drug as well as their mixtures. Thin square films of 3cmx3cm with a thickness of 0.7mm were cut from the dry sheet obtained by solvent evaporation. Coated films were prepared by dipping ACY and CDA drug-loaded EVA films (VA 40%) into EVA copolymer of VA 32% and then dried. All of the drug-loaded samples were extracted at 37 degrees C in 10ml distilled water that was replaced daily. The rate of individual drug release was measured by UV-spectrophotometer while the mixtures of drugs were measured by high performance liquid chromatography (HPLC).

RESULTS

The release rate of ACY is higher than that of CDA both individually and in the ACY/CDA 50/50 mixture. In the other mixtures, the release of the drug is proportional to its concentration in the mixture. Total release of ACY is higher than CDA in most compositions. The effect of increasing the vinyl acetate content of the EVA matrix increased the drug release rate (p=0.02) while coating of films resulted in a decrease of the release rate of the drugs.

SIGNIFICANCE

Measurements of the in vitro rate of drug release showed that there was a sustained release of drug at an almost constant concentration over extended period of time, thus providing a basis for oral treatment modality. We show that it is possible to alter the rate of drug release in the EVA matrix to a desired value by: (1) changing the composition of the EVA copolymer, (2) altering the mixtures of drugs and (3) coating the matrix with additional polymer. The use of mixtures of drugs that can enhance or decrease the rate of drug release may prove more effective in treating persistent oral infections in immunocompromised patients.

摘要

目的

本研究利用生物相容性乙烯-醋酸乙烯酯(EVA)共聚物在较长时间内以治疗水平递送药物。分别研究了抗真菌药阿昔洛韦(ACY)和抗菌药二醋酸氯己定(CDA)从EVA中的释放速率,以及它们作为混合物时的释放速率。阐述了药物组合、共聚物组成以及用不同聚合物对基质进行包衣对药物释放速率的影响。

方法

通过将EVA共聚物和药物按40:1的比例均匀溶解在二氯甲烷中制备聚合物浇铸溶液。ACY和CDA药物分别使用,并以三种不同的重量比使用,使聚合物中的总药物浓度保持在2.5%。在EVA基质中使用不同浓度的醋酸乙烯酯(VA)28%、32%和40%来研究单独的ACY或CDA的释放,而40%的VA用于研究单个药物及其混合物的释放。从通过溶剂蒸发得到的干燥片材上切割出3cm×3cm、厚度为0.7mm的方形薄膜。通过将负载ACY和CDA的EVA薄膜(VA 40%)浸入VA 32%的EVA共聚物中然后干燥来制备包衣薄膜。所有载药样品在37℃下于10ml每天更换的蒸馏水中萃取。单个药物的释放速率通过紫外分光光度计测量,而药物混合物通过高效液相色谱(HPLC)测量。

结果

ACY的释放速率在单独使用时以及在ACY/CDA 50/50混合物中均高于CDA。在其他混合物中,药物的释放与其在混合物中的浓度成正比。在大多数组成中,ACY的总释放量高于CDA。增加EVA基质中醋酸乙烯酯含量的效果提高了药物释放速率(p = 0.02),而薄膜包衣导致药物释放速率降低。

意义

体外药物释放速率的测量表明,在较长时间内药物以几乎恒定的浓度持续释放,从而为口服治疗方式提供了依据。我们表明,可以通过以下方式将EVA基质中的药物释放速率改变至所需值:(1)改变EVA共聚物的组成,(2)改变药物混合物,以及(3)用额外的聚合物对基质进行包衣。使用能够提高或降低药物释放速率的药物混合物可能在治疗免疫功能低下患者的持续性口腔感染方面更有效。

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