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将萜质体负载盐酸左西替利嗪凝胶作为耐甲氧西林金黄色葡萄球菌 (MRSA) 诱导的皮肤感染的重新定位治疗方法的整合; D-最优优化、离体、体内研究。

Integration of terpesomes loaded Levocetrizine dihydrochloride gel as a repurposed cure for Methicillin-Resistant Staphylococcus aureus (MRSA)-Induced skin infection; D-optimal optimization, ex-vivo, in-silico, and in-vivo studies.

机构信息

Department of Pharmaceutics, College of Pharmaceutical Sciences and Drug Manufacturing, Misr University for Science and Technology, Egypt.

Department of Pharmaceutics and Industrial Pharmacy, Faculty of Pharmacy, Cairo University, Egypt.

出版信息

Int J Pharm. 2023 Feb 25;633:122621. doi: 10.1016/j.ijpharm.2023.122621. Epub 2023 Jan 21.

DOI:10.1016/j.ijpharm.2023.122621
PMID:36693486
Abstract

The intention of this work is to assess the repurposed antimicrobial impact of Levocetirizine dihydrochloride (LVC), which is a well-known antihistaminic drug, in addition, to augment the antimicrobial effect by using terpene-enriched vesicles (TPs). To investigate how various parameters affect TPs aspects, TPs were made employing the ethanol-injection-method and optimized d-optimal design. The TPs were characterized based on their entrapment efficiency percentage (EE%), particle size (PS), polydispersity index (PDI), and zeta potential (ZP). The optimum TP was submitted to more examinations. The optimum TP (TP12) showed a spherical vesicle having an EE% of 66.39 ± 0.12%, PS of 243.3 ± 4.60 nm, PDI of 0.458 ± 0.003, and ZP of 24.2 ± 0.55 mV. The in-vitro release study results demonstrated that LVC is sustainedly liberated from the optimum TP compared to LVC-solution. The ex-vivo assessment showed that LVC was released in a more sustained manner from TPs-gel related to LVC solution, optimum TP, and LVC gel. Ex-vivo visualization by confocal laser scanning microscopy showed good deposition of the fluorescein-labeled TP. Further, the in-vitro anti-bacterial effect and biofilm inhibition and detachment assessment confirmed the potency of LVC against Methicillin-resistant-Staphylococcus-aureus (MRSA). The in-silico study demonstrated that the LVC has excellent stability with other ingredients combined with it in the TPs, further, it proved that LVC is a potential candidate for treating MRSA. In-vivo assessments revealed a good antimicrobial effect toward MRSA infection. Moreover, the histopathological evaluation confirmed the safety of using TPs-gel topically. In conclusion, MRSA-related skin infections may be treated using the LVC loaded TPs-gel as a promising system.

摘要

本工作旨在评估盐酸左西替利嗪(LVC)的再利用抗菌作用,LVC 是一种众所周知的抗组胺药物,此外,还通过使用富含萜烯的囊泡(TPs)来增强抗菌效果。为了研究各种参数如何影响 TPs 的各个方面,使用乙醇注入法和优化的 d-最优设计来制备 TPs。根据包封效率百分比(EE%)、粒径(PS)、多分散指数(PDI)和 Zeta 电位(ZP)对 TPs 进行了表征。对最佳 TPs 进行了更多的检查。最佳 TPs(TP12)呈球形囊泡,EE%为 66.39±0.12%,PS 为 243.3±4.60nm,PDI 为 0.458±0.003,ZP 为 24.2±0.55mV。体外释放研究结果表明,与 LVC 溶液相比,LVC 从最佳 TPs 中持续释放。离体评估表明,与 LVC 溶液、最佳 TP 和 LVC 凝胶相比,LVC 从 TPs-凝胶中以更持续的方式释放。共聚焦激光扫描显微镜的离体可视化显示,荧光素标记的 TP 得到了很好的沉积。此外,体外抗菌效果和生物膜抑制和脱落评估证实了 LVC 对耐甲氧西林金黄色葡萄球菌(MRSA)的功效。计算机研究表明,LVC 与 TPs 中的其他成分结合具有很好的稳定性,进一步证明 LVC 是治疗 MRSA 的潜在候选药物。体内评估显示对 MRSA 感染有良好的抗菌作用。此外,组织病理学评估证实了使用 TPs-凝胶进行局部治疗的安全性。总之,负载 LVC 的 TPs-凝胶可用于治疗 MRSA 相关的皮肤感染。

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