Formulation and In-Vitro, Ex-Vivo, and In-Vivo Evaluation of Mucoadhesive Buccal Tablets Containing Labetalol Hydrochloride for Enhancement of Systemic Bioavailability

Journal of Advanced Pharmacy Research Pub Date : 2022-01-01 DOI:10.21608/aprh.2021.97253.1142

Fatma Bakr, Moetaza M. Soliman, H. Elsabbagh

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引用次数: 1

Abstract

Objective: Labetalol hydrochloride is an alpha/beta adrenoceptor blocker that undergoes comprehensive first passmetabolism resulting in a low oral bioavailability. This study aimed to formulate and evaluate mucoadhesive buccal formulations of labetalol hydrochloride for enhancement of its bioavailability. Methods: Using various concentrations of hydroxypropyl methylcellulose (HPMC), carbopol-934, and sodium alginate, ten formulations of mucoadhesive buccal tablets containing labetalol hydrochloride were prepared. The produced tablets were evaluated to test physical and mucoadhesive properties as well as in-vitro drug release properties. Ex-vivo evaluations of the tablets were examined using chicken pouch membrane. Formulations that offered best results in in-vitro and ex-vivo evaluations were selected for running in-vivo comparative bioavailability study using New Zealand rabbits and adopted HPLC method to assess the buccal bioavailability of labetalol hydrochloride in relation to its oral bioavailability from commercial tablets. Results: It was found that drug release and mucoadhesive properties depended on the type and proportion of different polymers. Sodium alginate-containing formulations showed higher release rates and ex-vivo permeation rates compared to carbopolcontaining formulations. Increasing the proportion of HPMC resulted in more swelling, better mucoahesion forces and times but more delayed permeation and release rates. A strong correlation was detected between in-vivo drug release and ex-vivo transmucosal permeation of labetalol hydrochloride. The relative bioavailability of labetalol hydrochloride from the selected mucoadhesive buccal tablets F1 and F6 were 2.76 and 1.60, respectively. Conclusion: The produced mucoadhesive buccal tablets were successful in improving the systemic bioavailability of labetalol hydrochloride in rabbits. Clinical applications of formulations F1 and F6 are recommended.

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盐酸拉贝他洛尔黏附含片的配方及体外、离体和体内评价提高全身生物利用度

目的:盐酸拉贝他洛尔是一种α / β肾上腺素受体阻滞剂，经过全面的首次代谢导致口服生物利用度低。本研究旨在研制并评价盐酸拉贝他洛尔黏附口腔制剂，以提高其生物利用度。方法:以不同浓度的羟丙基甲基纤维素(HPMC)、卡波波-934、海藻酸钠为原料，制备含盐酸拉贝他洛尔黏附含片10种剂型。对所制片剂进行了物理性能、黏附性能和体外释药性能的评价。采用鸡囊膜法对片剂进行体外评价。选择体外和离体评价效果最佳的制剂进行新西兰兔体内比较生物利用度研究，采用高效液相色谱法评价盐酸拉贝他洛尔口腔生物利用度与市售片剂口服生物利用度的关系。结果:不同聚合物的种类和配比对药物释放和黏附性能有不同的影响。与含碳磷酸钠制剂相比，含海藻酸钠制剂具有更高的释放率和体外渗透率。增加HPMC的比例，肿胀程度增加，黏附力和黏附次数增加，但渗透和释放速度延迟。盐酸拉贝他洛尔体内药物释放与体外经粘膜渗透有很强的相关性。所得黏附口腔片F1和F6的相对生物利用度分别为2.76和1.60。结论:所制黏附含片能有效提高盐酸拉贝他洛尔在家兔体内的全身生物利用度。推荐配方F1、F6的临床应用。

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Journal of Advanced Pharmacy Research

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