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壳聚糖颊黏膜黏附贴片提高替扎尼定的系统生物利用度。

Chitosan-based buccal mucoadhesive patches to enhance the systemic bioavailability of tizanidine.

机构信息

Istanbul Medipol University, School of Pharmacy, Department of Pharmaceutical Technology, 34085, Istanbul, Türkiye.

University of Health Sciences, Faculty of Pharmacy, Department of Pharmaceutical Technology, 34668, Istanbul, Türkiye.

出版信息

Int J Pharm. 2023 Jul 25;642:123168. doi: 10.1016/j.ijpharm.2023.123168. Epub 2023 Jun 24.

Abstract

Tizanidine hydrochloride (TZN) is a muscle relaxant used to treat a variety of disorders such as painful muscle spasms and chronic spasticity. TZN has low oral bioavailability due to extensive first-pass metabolism and is used orally at a dose of 6-24 mg per day. In the present study, buccal patches were prepared by solvent casting method using chitosan glutamate (Chi-Glu) and novel chitosan azelate (Chi-Aze) which was synthesised in-house for the first time, to enhance the bioavailability of TZN by bypassing first-pass metabolism. The characterisation, mucoadhesion and drug release studies were performed. Chi-Aze patches retained their integrity longer in the buccal medium and showed higher ex vivo drug permeability compared to that prepared with Chi-Glu. In vivo studies revealed that buccal formulation fabricated with Chi-Aze (3%) showed approx 3 times more bioavailability than the orally administered commercial product. Results of the studies indicate that Chi-Aze, prepared by conjugation of chitosan and a fatty acid, the patch formulation is a promising buccal mucoadhesive system due to the physical stability in buccal medium, the good mucoadhesiveness and the high TZN bioavailability. Moreover, Chi-Aze patch might be an alternative to oral formulations of TZN to reduce the dose and frequency of drug administration.

摘要

盐酸替扎尼定(TZN)是一种肌肉松弛剂,用于治疗多种疾病,如疼痛性肌肉痉挛和慢性痉挛。由于广泛的首过代谢,TZN 的口服生物利用度较低,每天口服剂量为 6-24mg。在本研究中,通过溶剂浇铸法制备了颊贴片,使用了壳聚糖谷氨酸(Chi-Glu)和我们首次合成的新型壳聚糖己二酸酯(Chi-Aze),以通过绕过首过代谢来提高 TZN 的生物利用度。进行了特征描述、粘膜粘附和药物释放研究。与用 Chi-Glu 制备的贴片相比,Chi-Aze 贴片在颊介质中保持完整性的时间更长,并且显示出更高的体外药物渗透性。体内研究表明,用 Chi-Aze(3%)制备的颊制剂的生物利用度比口服商业产品高约 3 倍。研究结果表明,通过壳聚糖和脂肪酸的缀合制备的 Chi-Aze,这种贴片制剂是一种有前途的颊粘膜粘附系统,因为它在颊介质中具有物理稳定性、良好的粘膜粘附性和高 TZN 生物利用度。此外,Chi-Aze 贴片可能是 TZN 口服制剂的替代品,以减少药物的剂量和给药频率。

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