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用于改善渗透和皮肤滞留的载阿普米拉斯溶致液晶纳米颗粒包埋水凝胶:一种治疗银屑病的有效方法。

Apremilast loaded lyotropic liquid crystalline nanoparticles embedded hydrogel for improved permeation and skin retention: An effective approach for psoriasis treatment.

作者信息

Rapalli Vamshi Krishna, Tomar Yashika, Sharma Swati, Roy Aniruddha, Singhvi Gautam

机构信息

Department of Pharmacy, Birla Institute of Technology and Science, Pilani 333031, India.

Department of Pharmacy, Birla Institute of Technology and Science, Pilani 333031, India.

出版信息

Biomed Pharmacother. 2023 Jun;162:114634. doi: 10.1016/j.biopha.2023.114634. Epub 2023 Apr 3.

DOI:10.1016/j.biopha.2023.114634
PMID:37018989
Abstract

The present work aimed to prepare and evaluate Apremilast loaded lyotropic liquid crystalline nanoparticles (LCNPs) formulation for skin delivery to enhance the efficacy with reduced adverse effects of the oral therapy in psoriasis treatment. The LCNPs were prepared using the emulsification using a high shear homogenizer for size reduction and optimized with Box Behnken design to achieve desired particle size and entrapment efficiency. The selected LCNPs formulation was evaluated for in-vitro release, in-vitro psoriasis efficacy, skin retention, dermatokinetic, in-vivo skin retention, and skin irritation study. The selected formulation exhibited 173.25 ± 2.192 nm (polydispersity 0.273 ± 0.008) particle size and 75.028 ± 0.235% entrapment efficiency. The in-vitro drug release showed the prolonged-release for 18 h. The ex-vivo studies revealed that LCNPs formulation exhibited drug retention up to 3.2 and 11.9-fold higher, in stratum corneum and viable epidermis compared to conventional gel preparation. In-vitro cell line studies performed on immortal keratinocyte cells (HaCaT cells) demonstrated non-toxicity of selected excipients used in designed LCNPs. The dermatokinetic study revealed the AUC of the LCNPs loaded gel was 8.4 fold higher in epidermis and 2.06 fold in dermis, respectively compared to plain gel. Further, in-vivo animal studies showed enhanced skin permeation and retention of Apremilast compared to conventional gel.

摘要

本研究旨在制备并评估用于皮肤给药的阿普米拉斯溶致液晶纳米粒(LCNPs)制剂,以提高其在银屑病治疗中的疗效,同时减少口服治疗的不良反应。使用高剪切均质机通过乳化法制备LCNPs以减小粒径,并采用Box Behnken设计进行优化,以达到所需的粒径和包封率。对所选的LCNPs制剂进行体外释放、体外银屑病疗效、皮肤滞留、皮肤动力学、体内皮肤滞留和皮肤刺激性研究。所选制剂的粒径为173.25±2.192 nm(多分散性0.273±0.008),包封率为75.028±0.235%。体外药物释放显示其具有18小时的缓释效果。体外研究表明,与传统凝胶制剂相比,LCNPs制剂在角质层和活表皮中的药物滞留量分别高出3.2倍和11.9倍。对永生化角质形成细胞(HaCaT细胞)进行的体外细胞系研究表明,设计的LCNPs中使用的所选辅料无毒性。皮肤动力学研究表明,与普通凝胶相比,载有LCNPs的凝胶在表皮中的AUC分别高出8.4倍,在真皮中的AUC高出2.06倍。此外,体内动物研究表明,与传统凝胶相比,阿普米拉斯的皮肤渗透和滞留得到增强。

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