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负载百里酚的基于Eudragit RS30D阳离子纳米颗粒的水凝胶在伤口局部应用中的体外和体内评价

Thymol-Loaded Eudragit RS30D Cationic Nanoparticles-Based Hydrogels for Topical Application in Wounds: In Vitro and In Vivo Evaluation.

作者信息

Mohsen Amira Mohamed, Nagy Yosra Ibrahim, Shehabeldine Amr M, Okba Mona M

机构信息

Pharmaceutical Technology Department, National Research Centre, El-Buhouth Street, Dokki, Cairo 12622, Egypt.

Department of Microbiology and Immunology, Faculty of Pharmacy, Cairo University, Cairo 11562, Egypt.

出版信息

Pharmaceutics. 2022 Dec 21;15(1):19. doi: 10.3390/pharmaceutics15010019.

Abstract

Natural medicines formulated using nanotechnology-based systems are a rich source of new wound-treating therapeutics. This study aims to develop thymol-loaded cationic polymeric nanoparticles (CPNPs) to enhance the skin retention and wound healing efficacy of thymol. The developed materials exhibited entrapment efficiencies of 56.58 to 68.97%, particle sizes of 36.30 to 99.41 nm, and positively charged zeta potential. In Vitro sustained release of thymol up to 24 h was achieved. Selected thymol CPNPs (F5 and C2) were mixed with methylcellulose to form hydrogels (GF5 and GC2). An In Vivo skin-retention study revealed that GF5 and GC2 showed 3.3- and 3.6-fold higher retention than free thymol, respectively. An In Vitro scratch-wound healing assay revealed a significant acceleration in wound closure at 24 h by 58.09% (GF5) and 57.45% (GC2). The potential for free thymol hydrogel, GF5, and GC2 to combat MRSA in a murine skin model was evaluated. The bacterial counts, recovered from skin lesions and the spleen, were assessed. Although a significant reduction in the bacterial counts recovered from the skin lesions was shown by all three formulations, only GF5 and GC2 were able to reduce the bacterial dissemination to the spleen. Thus, our study suggests that Eudragit RS30D nanoparticles-based hydrogels are a potential delivery system for enhancing thymol skin retention and wound healing activity.

摘要

使用基于纳米技术的系统配制的天然药物是新型伤口治疗疗法的丰富来源。本研究旨在开发负载百里酚的阳离子聚合物纳米颗粒(CPNP),以提高百里酚在皮肤中的保留率和伤口愈合效果。所制备的材料包封率为56.58%至68.97%,粒径为36.30至99.41nm,且具有带正电荷的ζ电位。实现了百里酚在体外长达24小时的持续释放。将选定的百里酚CPNP(F5和C2)与甲基纤维素混合以形成水凝胶(GF5和GC2)。体内皮肤保留研究表明,GF5和GC2的保留率分别比游离百里酚高3.3倍和3.6倍。体外划痕伤口愈合试验表明,在24小时时伤口闭合显著加速,GF5组加速了58.09%,GC2组加速了57.45%。评估了游离百里酚水凝胶、GF5和GC2在小鼠皮肤模型中对抗耐甲氧西林金黄色葡萄球菌(MRSA)的潜力。对从皮肤损伤处和脾脏中回收的细菌数量进行了评估。尽管所有三种制剂均显示从皮肤损伤处回收的细菌数量显著减少,但只有GF5和GC2能够减少细菌向脾脏的扩散。因此,我们的研究表明,基于Eudragit RS30D纳米颗粒的水凝胶是一种潜在的递送系统,可增强百里酚在皮肤中的保留率和伤口愈合活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9661/9861126/084055e13884/pharmaceutics-15-00019-g001.jpg

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