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盐酸曲马多载壳聚糖纳米粒经鼻腔给药:制剂、特性及其体内评价。

Intranasal delivery of tapentadol hydrochloride-loaded chitosan nanoparticles: formulation, characterisation and its in vivo evaluation.

机构信息

a Faculty of Pharmacy , The Maharaja Sayajirao University of Baroda , Vadodara , India.

出版信息

J Microencapsul. 2017 Nov;34(7):644-658. doi: 10.1080/02652048.2017.1375038. Epub 2017 Sep 18.

Abstract

The aim of the present investigation was to formulate tapentadol hydrochloride-loaded chitosan nanoparticles (CS-NPs) for nose to brain delivery. Chitosan nanoparticles were prepared using ionotropic gelation technique. Optimisation of the formulation and process parameters was done using Box-Behnken Design. The entrapment efficiency, drug loading, Z-average size and zeta potential of the optimised batch were 63.49 ± 1.61%, 17.25 ± 1.38%w/w, 201.2 ± 1.5 nm and +49.3 mV, respectively. In-vitro release study showed 84.04 ± 1.53% drug release after 28 h, while ex vivo studies indicated higher permeation of CS-NPs through nasal mucosa. The nanoparticles exhibited good mucoadhesiveness, haemocompatibility and safety as evidenced by histopathology. The results of the pharmacodynamic study revealed prolongation of the analgesic activity. The intranasal instillation of CS-NPs resulted in the higher concentrations in brain compared to the drug solution and intravenous administration of CS-NPs. In a nutshell, intranasal administration of tapentadol hydrochloride-loaded CS-NPs is a promising approach for effective pain management.

摘要

本研究旨在制备盐酸曲马多载壳聚糖纳米粒(CS-NPs)用于经鼻递药。采用离子凝胶化技术制备壳聚糖纳米粒。采用 Box-Behnken 设计优化处方和工艺参数。优化批次的包封效率、载药量、Z 均粒径和 Zeta 电位分别为 63.49±1.61%、17.25±1.38%w/w、201.2±1.5nm 和+49.3mV。体外释放研究显示,28 小时后药物释放 84.04±1.53%,而体外研究表明 CS-NPs 经鼻黏膜的渗透性更高。纳米粒表现出良好的黏膜黏附性、血液相容性和安全性,组织病理学证实了这一点。药效学研究结果表明,镇痛活性延长。与药物溶液和 CS-NPs 的静脉给药相比,CS-NPs 的经鼻滴注导致脑内浓度更高。总之,盐酸曲马多载壳聚糖纳米粒经鼻给药是一种有前途的有效疼痛管理方法。

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