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A polymeric device for delivery of anti-microbial and anti-fungal drugs in the oral environment: effect of temperature and medium on the rate of drug release

机译:用于在口腔环境中递送抗微生物和抗真菌药物的聚合物装置:温度和介质对药物释放速率的影响

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摘要

Objectives. The use of drag delivery systems in dentistry is a relatively new area of research with the exception of fluoride ion release from polyalkenoate cements and their predecessor silicate cements. The present study is based on the use of a bio-compatible material ethylene vinyl acetate copolymer (EVA) that enables constant release of drugs of therapeutic levels over extended periods of time at doses suitable for the treatment of oral conditions. Method. Polymer casting solutions were made by dissolving EVA and the drug in the ratio of 40:1 in 70 ml of dichloromethane at 38 ℃ for 6 h. Thin square films of 3 X 3 cm~2 with a thickness of 1 mm were cut from the dry sheet obtained by solvent evaporation technique. Drug loaded samples were extracted for a minimum of 14 days in 10 ml medium (double distilled water or water/ethanol (4:1)) which was replaced daily. Spectral measurements were made to follow changes in optical densities (OD) during release kinetics. Effect of temperature (24 and 37 ℃) on the rate of drug release was studied and the energies of activation (ΔE~≠) were calculated using Arrehenius equation for the diffusion (translocation) of molecules of tetracycline hydrochloride (TTH), doxycycline hydrochloride (DOH), and chlorhexidine diacetate (CDA) in water as extracting medium. Effect of extracting medium (water and water/ethanol (4:1)) was also investigated on the rate of drug release measurements at 24 ℃. Results. Analysis of variance of the data revealed that significantly enhanced rates were observed at the higher temperature (37 ℃) and when extracting medium was changed to water/ethanol (4:1) for TTH, DOH and CDA (p < 0.0015). The enhanced rate values seem to be due to the formation of channels in the polymer. The largest activation energy (21.83 kcal mol~(-1)) observed for CDA was interpreted as due to the highest average molecular weight (626) compared to TTH (481) and DOH (481). Significance. These in vitro rate of drug release measurements will provide a basis for establishing a novel approach (treatment modality) for sustained intra-oral drug delivery over extended time periods using laboratory methods and materials that are readily available to dentists.
机译:目标。除了从聚链烯酸酯水泥及其前身的硅酸盐水泥中释放氟离子外,在牙科领域中使用阻力输送系统是一个相对较新的研究领域。本研究基于生物相容性材料乙烯乙酸乙烯酯共聚物(EVA)的使用,该共聚物能够以适合口服条件的剂量在较长的时间内持续释放治疗水平的药物。方法。将EVA和药物以40:1的比例在38℃的70 ml二氯甲烷中溶解6小时制成聚合物浇铸溶液。从通过溶剂蒸发技术获得的干燥片上切下厚度为1mm的3×3cm 2的正方形薄薄膜。在10毫升培养基(双蒸馏水或水/乙醇(4:1))中提取载药样品至少14天,每天更换一次。进行光谱测量以跟踪释放动力学期间光密度(OD)的变化。研究了温度(24和37℃)对药物释放速率的影响,并使用Arrehenius方程计算了四环素盐酸盐(TTH),强力霉素盐酸盐(TTH)分子的扩散(易位)的活化能(ΔE〜≠)。 DOH)和二乙酸氯己定(CDA)作为萃取介质。还研究了萃取介质(水和水/乙醇(4:1))对24℃药物释放速率的影响。结果。数据方差分析表明,在较高温度(37℃)下,当TTH,DOH和CDA的萃取介质改为水/乙醇(4:1)时,观察到的速率显着提高(p <0.0015)。速率值的提高似乎是由于聚合物中形成了通道。 CDA观察到的最大活化能(21.83 kcal mol〜(-1))被解释为与TTH(481)和DOH(481)相比具有最高的平均分子量(626)。意义。这些体外药物释放速率的测量将为建立新方法(治疗方式)奠定基础,该新方法可使用实验室方法和牙医容易获得的材料在延长的时间段内持续口服药物。

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