Potential of Cocoa Pod Husk Pectin-Based Modified Release Capsules as a Carrier for Chronodelivery of Hydrocortisone in Sprague-Dawley Rats.

Journal of drug delivery Pub Date : 2018-10-08 eCollection Date: 2018-01-01 DOI:10.1155/2018/9825363
Ofosua Adi-Dako, Kwabena Ofori-Kwakye, Seth Kwabena Amponsah, Isaac Boamah, Noble Kuntworbe, Esther Eshun Oppong
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引用次数: 5

Abstract

The potential of cocoa pod husk (CPH) pectin-based modified release (MR) capsules as a carrier for chronodelivery of hydrocortisone in Sprague-Dawley rats was assessed. Extemporaneously formulated CPH pectin-based hydrocortisone (10 mg) capsules crosslinked with calcium chloride (Formulation A) or zinc (Formulation B) and a commercial immediate release hydrocortisone formulation were administered orally to Sprague-Dawley rats and the pharmacokinetic parameters were evaluated using noncompartmental analysis. Formulation A had a 2 h lag phase followed by an increase in serum drug concentration in the treated rats. Peak concentrations (Cmax) of 21.799 ± 1.993 ng/ml and 20.844 ± 2.661 ng/ml were achieved after 6 ± 0.23 h and 6 ± 0.35 h (Tmax), respectively, for capsules A and B. The immediate release formulation had a peak concentration of 15.322 ± 0.313 ng/ml within 1 ± 0.2 h. The relative bioavailability of the CPH pectin-based capsules A and B was 213% and 274%, respectively. Formulations A and B had half-lives more than three times that of the immediate release formulation. The MR capsules exhibited a higher exposure, greater bioavailability, and versatility in release of cortisol than the commercial immediate release formulation. Additionally, the MR capsules exhibited an extended drug release with overnight cortisol rise and early morning cortisol peak and hold promise in the management of adrenal insufficiency.

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可可荚壳果胶基改性释放胶囊作为大鼠慢性递送氢化可的松载体的潜力。
研究了可可豆荚壳(CPH)果胶基改性释放胶囊(MR)作为Sprague-Dawley大鼠慢性递送氢化可的松载体的潜力。将临时配制的CPH果胶为基础的氢化可的松(10 mg)胶囊与氯化钙(配方A)或锌(配方B)交联,以及一种商业速释氢化可的松胶囊口服给药于Sprague-Dawley大鼠,并采用非室室分析评估药代动力学参数。制剂A在给药大鼠体内有2小时的滞后期,随后血清药物浓度升高。A胶囊和b胶囊在6±0.23 h和6±0.35 h (Tmax)后的峰浓度(Cmax)分别为21.799±1.993 ng/ml和20.844±2.661 ng/ml;速释制剂在1±0.2 h内的峰浓度为15.322±0.313 ng/ml。CPH果胶基胶囊A和B的相对生物利用度分别为213%和274%。制剂A和B的半衰期是立即释放制剂的三倍以上。MR胶囊比商业即刻释放制剂表现出更高的暴露、更高的生物利用度和释放皮质醇的多功能性。此外,MR胶囊在夜间皮质醇升高和清晨皮质醇峰值时表现出延长的药物释放,并有望治疗肾上腺功能不全。
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
Journal of drug delivery
Journal of drug delivery PHARMACOLOGY & PHARMACY-
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