Evaluation of the matrix-forming ability of Chrysophyllum albidum Linn fruit gum in sustained-release tablet formulations

IF 0.7 Q4 PHARMACOLOGY & PHARMACY Journal of Reports in Pharmaceutical Sciences Pub Date : 2021-01-01 DOI:10.4103/jrptps.JRPTPS_13_20
Ephraim Esla, O. Olayemi, B. Isah, S. Allagh
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Abstract

Background: Plant gums are extensively being exploited as pharmaceutical excipients due to the ease of availability, biodegradability, and reduced costs. Aim: This study investigated the application of the fruit gum of Crysophyllum albidum (CFG) as a matrix former in the formulation of chlorpheniramine maleate and theophylline hydrochloride tablets. Materials and Methods: The gum was extracted using acetone and evaluated for flow, swelling, and hydration capacity. Effects of temperature on CFG and drug compatibility were evaluated using differential scanning calorimetry (DSC). Granules containing CFG at 10, 20, and 30% w/w were prepared using the wet granulation method and evaluated for flow properties. Compressed tablets were evaluated for uniformity of weight, hardness, friability, and drug content. In vitro drug release studies were carried out in simulated gastric (pH 1.2) and simulated intestinal (pH 6.8) fluids. Pearson’s similarity correlations were used to analyze results. Results: CFG had a swelling capacity of 22% and hydration capacity of 1.44 with an angle of repose of 30o and Carr’s index of 7.6 signifying good flow. DSC thermogram returned an endothermic glass transition peak at 72.1oC with no appreciable shifts in the peak when CFG was incorporated into the drug. Tablet hardness and friability were concentration dependent with values of 6.5–8.5kg F and 0.04–0.4%, respectively; drug content was within official specifications. Formulations containing 30%w/w CFG sustained drug release for over 12 h and showed better ability to control drug release than HPMC at same concentration. Conclusion: This study shows the propensity of CFG to be used in the formulation of sustained-release tablet formulations.
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白叶果胶缓释片基质形成能力的评价
背景:植物胶因其易得性、生物降解性和降低成本而被广泛用作药用辅料。目的:研究白水晶果胶作为基质形成剂在马来酸氯苯那敏和盐酸茶碱片中的应用。材料和方法:用丙酮提取树胶,并评估其流动性、溶胀性和水合能力。用差示扫描量热法(DSC)评价了温度对CFG及药物相容性的影响。使用湿法制粒法制备含有10%w/w、20%w/w和30%w/w CFG的颗粒,并评估其流动特性。对压片的重量、硬度、脆性和药物含量的均匀性进行了评估。在模拟胃液(pH 1.2)和模拟肠液(pH 6.8)中进行体外药物释放研究。使用Pearson相似性相关性对结果进行分析。结果:CFG具有22%的溶胀能力和1.44的水化能力,休止角为30o,Carr指数为7.6,表明其具有良好的流动性。DSC热谱图在72.1oC处返回吸热玻璃化转变峰,当CFG掺入药物时该峰没有明显的变化。片剂硬度和脆性与浓度有关,分别为6.5–8.5kg F和0.04–0.4%;药物含量符合官方规定。含有30%w/w CFG的制剂持续药物释放超过12 h,并且在相同浓度下表现出比HPMC更好的控制药物释放的能力。结论:本研究显示了CFG在缓释片制剂中的应用潜力。
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来源期刊
Journal of Reports in Pharmaceutical Sciences
Journal of Reports in Pharmaceutical Sciences Pharmacology, Toxicology and Pharmaceutics-Pharmacology, Toxicology and Pharmaceutics (all)
CiteScore
1.40
自引率
0.00%
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0
期刊介绍: The Journal of Reports in Pharmaceutical Sciences(JRPS) is a biannually peer-reviewed multi-disciplinary pharmaceutical publication to serve as a means for scientific information exchange in the international pharmaceutical forum. It accepts novel findings that contribute to advancement of scientific knowledge in pharmaceutical fields that not published or under consideration for publication anywhere else for publication in JRPS as original research article. all aspects of pharmaceutical sciences consist of medicinal chemistry, molecular modeling, drug design, pharmaceutics, biopharmacy, pharmaceutical nanotechnology, pharmacognosy, natural products, pharmaceutical biotechnology, pharmacology, toxicology and clinical pharmacy.
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