In-Vivo Pharmacokinetics Study of Exemestane Hydrochloride Self-nanoemulsifying Drug Delivery Systems via Oral Route

Letters in Applied NanoBioScience Pub Date : 2022-09-17 DOI:10.33263/lianbs124.098

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Abstract

Exemestane HCl (EXM) is a novel irreversible steroidal aromatase inhibitor for the adjuvant treatment of hormonally responsive breast cancer in postmenopausal women. Poor aqueous solubility of EXM is the biggest hurdle for developing solid oral dosage forms. That’s why the current study aims to evaluate the pharmacokinetics of formulating the EXM loaded self nano emulsifying drug delivery (SNEDDs) system. SNEDDs were formulated using Labrafac CC (20% w/v), Tween 80 (27%w/v), and Triacetin (54%w/v) as oil, surfactant, and co-surfactant, respectively, by water titration method. A comparative Pharmacokinetics study of EXM suspension and EXM SNEDDS was performed using a female waster rate. The developed formulation had a 37.65± 5.08 nm size and a 21.57±0.73 sec of self-emulsification time. Cmax of EXM suspension and EXM SNEDDS was found to be 122.49±8.27 and 194.86 ± 14.75 ng/mL, respectively. AUC0-720 of EMX SNEDDS was 1.71 times higher compared to EXM suspension, indicating that lipid nanoparticles improve the drug concentration in the plasma. So we conclude that SNEDDS improves the pharmacokinetic of EXM, which subsequently improves oral bioavailability.

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盐酸依西美坦自纳米乳化给药系统的体内药代动力学研究

依西美坦HCl (EXM)是一种新型的不可逆甾体芳香酶抑制剂，用于绝经后妇女激素反应性乳腺癌的辅助治疗。EXM的水溶性差是开发固体口服剂型的最大障碍。这就是为什么本研究旨在评估构建EXM负载的自纳米乳化给药系统的药代动力学。分别以Labrafac CC (20% w/v)、Tween 80 (27%w/v)和Triacetin (54%w/v)为油、表面活性剂和助表面活性剂，采用水滴定法配制snedd。使用女性废物率对EXM悬浮液和EXM SNEDDS进行了比较药代动力学研究。该配方粒径为37.65±5.08 nm，自乳化时间为21.57±0.73秒。EXM混悬液和EXM SNEDDS的Cmax分别为122.49±8.27和194.86±14.75 ng/mL。EMX SNEDDS的AUC0-720比EXM悬液高1.71倍，表明脂质纳米颗粒提高了血浆中药物浓度。因此，我们得出结论，SNEDDS改善了EXM的药代动力学，从而提高了口服生物利用度。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Letters in Applied NanoBioScience

CiteScore

2.40

自引率

0.00%

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