提高溶解度的替卡格雷片自微乳化体系的配制与表征

Q4 Medicine International journal of pharmaceutical compounding Pub Date : 2024-05-01
Rajagopal Kumaravelrajan, Narayanan Naresh, Guru Prasad Mohanta, Suba Venkatesan, Pasupuleti Dharani Prasad
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引用次数: 0

摘要

替卡格雷用于抑制急性冠状动脉综合征,但其溶解性差和生物利用度低限制了其体内疗效。本研究的目的是制造一种优化的片剂形式的替卡格雷负载型自微乳化给药系统,以提高该药物的溶解度和溶出度。为确定本研究中油的浑浊程度进行了初步研究,并使用假三元相图确定了三种比例(1:1、1:2 和 1:3)的微乳液形成区域。用选定的油和表面活性剂与共表面活性剂混合物测定了替卡格雷的溶解度。微乳剂的复配采用了简单点阵混合物设计。经过沉淀研究后,使用吸附剂(气溶胶)将微乳剂转化为颗粒剂。经过表征后,将颗粒压制成片剂,进行体外释放研究。对优化配方进行了各种表征程序,以确定其 zeta 电位、粒度和表面形态。结果发现,在所有配方中,药物的溶解度都增加了许多倍,优化配方的溶解度为 221.37 毫克/毫升。关于替卡格雷片剂,在自微乳化给药系统中需要高达 30% 的气溶胶作为吸附剂。对替卡格雷颗粒的压片效果令人满意。在所有配方中,活性药物在 30 分钟溶解时间内的释放率均超过 80%。优化后的西格列洛自微乳化给药系统配方由中链甘油三酯油(47.88.0%)、表面活性剂(28.25%)和助表面活性剂(23.85%)组成,显著提高了西格列洛的溶解度。扫描电子显微镜的分析结果表明,药物的表面和尺寸以及 zeta 电位也令人满意,这表明本报告中描述的优化的替卡格雷负载型自微乳化给药系统可成功用作实现替卡格雷溶出增强的有效方法。
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Compounding and Characterization of a Selfmicroemulsifying System of Ticagrelor Tablets for Enhanced Solubility.

Ticagrelor is used to inhibit acute coronary syndrome, but its poor solubility and low bioavailability limit its in-vivo efficacy. The purpose of this study was to manufacture an optimized ticagrelor-loaded self-microemulsifying drug-delivery system in the form of tablets to enhance the solubility and dissolution of that drug. A preliminary study was conducted to determine the extent of turbidity of oils for this study, and a pseudoternaryphase diagram was used to identify the region of formation of microemulsion with 3 ratios (1:1,1:2, and 1:3). The solubility of ticagrelor was determined with the selected oil and a surfactant-and-cosurfactant mixture. A simplex lattice mixture design was used to compound the microemulsion. The microemulsion was converted to granules by the use of an adsorbent (aerosol) after a precipitation study. After characterization, the resultant granules were compressed into tablets for an in-vitro release study. The optimized formulation was subjected to various characterization procedures to determine the zeta potential, particle size, and surface morphology. The solubility of the drug was found to have increased manyfold in all formulations, and the optimized formulation was found to be 221.37 mg/mL. With respect to the ticagrelor tablets, aerosol up to 30% was needed as an adsorbent in the self-microemulsifying drug-delivery system. The compression of the ticagrelor granules was satisfactory for tablet formation. In all formulations, the release of the active drug was more than 80% within 30 minutes of dissolution time. The optimized icagrelorloaded self-microemulsifying drug-delivery system formulation consisted of medium-chain triglyceride oil (47.88.0%), surfactant (28.25%), and cosurfactant (23.85%), which significantly improved the dissolution of ticagrelor. The results of analysis via scanning electron microscopy revealed that the surface and size of the drug and the zeta potential were also satisfactory and suggested that the optimized ticagrelor-loaded self-microemulsifying drug-delivery system described in this report could be successfully used as an efficient method for achieving enhanced dissolution of ticagrelor.

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来源期刊
CiteScore
0.40
自引率
0.00%
发文量
62
期刊介绍: The International Journal of Pharmaceutical Compounding (IJPC) is a bi-monthly, scientific and professional journal emphasizing quality pharmaceutical compounding. IJPC is the only publication that covers pharmaceutical compounding topics relevant and necessary to empower pharmacists to meet the needs of today"s patients. No other publication features hands-on, how-to compounding techniques or the information that contemporary pharmacists need to provide individualized care.
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