Cefotaxime Combined Ellagic Acid in a Liposomal Form for More Stable and Antimicrobial Effective Formula

Hani Asfour
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引用次数: 5

Abstract

The aim of this study is loading of cefotaxime (CXM) and ellagic acid (EA) in a liposomal formula to enhance CXM corneal permeability, stability and antimicrobial activity, thin film hydration method used to form CXM- EA liposomes, particle size, zeta potential, scan electron microscope image, CXM release, drug stability and antimicrobial activity were tested. CTX entrapped in CXM – EA liposomes was 42.1 ± 3.2%, ellagic acid content was 72.1 ± 3.1%, particle size was 251.7 ± 1.2 nm, and Zeta potential was 12.4 ± 3.1 mV with a polydispersity index of 0.34 ± 0.21.In concern to CXM released, it was a dramatic rapid diffusion of raw CXM (~88%) after 1 hour, however, CXM released from CXM –EA liposomes (~50 %), after 2 h, raw CXM was completely dissolved in the buffer medium, but it takes about 8 h to be completely released to the buffered medium. Stability study was carried out among 14 days at room and refrigerator temperatures, raw CXM was expired after 7 days while the formulated CXM content was (~93 %) and (~96 %) for room and refrigerator temperature respectively, finally, antimicrobial activity was carried out against two gram positive and two gram negative microorganisms, data revealed that ellagic acid potentiates the antimicrobial activity of CXM.
头孢噻肟复合鞣花酸脂质体制备稳定有效的抗菌配方
本研究的目的是在脂质体中负载头孢噻肟(CXM)和鞣花酸(EA)来增强CXM的角膜渗透性、稳定性和抗菌活性,采用薄膜水合法形成CXM- EA脂质体,对其粒径、zeta电位、扫描电镜图像、CXM的释放、药物稳定性和抗菌活性进行测试。CXM - EA脂质体的CTX包封率为42.1±3.2%,鞣花酸含量为72.1±3.1%,粒径为251.7±1.2 nm, Zeta电位为12.4±3.1 mV,多分散指数为0.34±0.21。对于CXM的释放,1 h后CXM的快速扩散(~88%),而CXM -EA脂质体释放的CXM (~ 50%), 2 h后CXM完全溶解在缓冲介质中,但需要8 h左右才能完全释放到缓冲介质中。在室温和冷藏条件下进行了14 d的稳定性研究,在室温和冷藏条件下配制的CXM含量分别为(~ 93%)和(~ 96%),7 d后过期,最后对两种革兰氏阳性和两种革兰氏阴性微生物进行了抑菌活性研究,结果表明鞣花酸增强了CXM的抑菌活性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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