Technology Criteria for the Manufacturing of Rebamipide Film-coated Tablets

G. V. Trusov, B. V. Brovchenko, Z. M. Kozlova, I. Krasnyuk
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Abstract

Introduction. The current growth of the pharmaceutical market and stiff competition require from drug manufacturers make a more detailed and thorough fine-tuning of existing production lines. Direct compression technology is a modern and cost-effective technology for solid dosage form drug manufacturing. Roll-compaction tehnology (dry granulation) can be an alternative approach to optimize the manufacturing of formulations, for which the use of wet granulation or direct compression technologies is not possible due to their physical and chemical properties.Aim. The goal of this work is to investigate the possibility of manufacturing Rebamipide tablets by using direct compression technology and dry granulation technology (roll-compaction), avoiding such complicated and more ex-pensive technology as wet granulation. Also aim of this work is study the impact of production methods on such quality factors as disintegration and dis-solution time.Materials and methods. In this study were used such materials as Rebamipide substance (α-[(4-Chlorobenzoyl)amino]-1,2-dihydro-2-oxo-4-quinolinepropanoic acid) (experimental sample), MCC-102 (J. Rettenmaier & Söhne (JRS), Germany), Starch pregelatinized (Colorcon LTD., England), Kollidone SR (BASF, Germany), Croscarmellose sodium (J. Rettenmaier & Söhne (JRS), Germany), Anhydrous citric acid (Scharlau), Sodium lauryl sulfate (BASF, Germany), Aerosil 200 vv Pharma (Evonik Industries AG, Germany), Sodium stearyl fumarate (J. Rettenmaier & Söhne (JRS), Germany), Calcium stearate (FACI, Italy), Film coating VIVACOAT® PA-1P-000 (J. Rettenmaier & Söhne (JRS), Germany). Also were used such equipment as Y shape blender («AZT FARMA K.B.», Russia), roll compactor LGC100 (Beijing Gylongli Automation Tech. Co., Ltd, China), rotary tablet press PG16G (Beijing Gylongli Automation Tech. Co., Ltd, China), tablet coating system Labcoat™ M (O'Hara Technologies lnc, Canada), ionising air gun Simco Cobra (SimcoIon, Netherlands), flowability tester ERWEKA GT (ERWEKA GmbH, Germany), powder density tester ERWEKA SVM 122 (ERWEKA GmbH, Germany), vibrating sieve CISA RP 200N (CISA Cedaceria Industrial S.L., Spain), tablet hardness, thickness and height tester SOTAX HT 10 (SOTAX AG, Switzerland), dissolution tester DT 626/1000HH (ERWEKA GmbH, Germany) and disintegration tester ZT321 (ERWEKA GmbH, Germany).Results and discussion. In a series of experiments were obtained tablet’s cores and film coated tablets by direct compression and roll-compaction methods. Experimentally it was found, that in tablets with similar formulations roller compaction technology provides slower disintegration and dissolution time, compared to direct compression method. This fact should be taken into account during drug development when planning the rate of release of the active ingredient.Conclusion. As a result of the experiments it was shown a direct correlation between the use of a certain technology and its impact in such quality indicators as disintegration and dissolution time of tablets. It was also found that dry granulation technology provides a more technologically suitable tablet mass.
生产雷巴米特薄膜衣片的技术标准
引言当前医药市场的增长和激烈的竞争要求药品生产商对现有生产线进行更细致、更彻底的微调。直接压制技术是一种经济有效的现代固体制剂生产技术。辊压技术(干法制粒)是优化制剂生产的另一种方法,由于其物理和化学特性,湿法制粒或直接压缩技术无法用于制剂生产。这项工作的目的是研究使用直接压缩技术和干法制粒技术(辊压)生产雷巴米特片剂的可能性,避免使用湿法制粒这种复杂而昂贵的技术。这项工作的另一个目的是研究生产方法对崩解和溶解时间等质量因素的影响。本研究使用的材料包括雷巴米特物质(α-[(4-氯苯甲酰基)氨基]-1,2-二氢-2-氧代-4-喹啉丙酸)(实验样品)、MCC-102(J. Rettenmaier & Söhne(JRS),德国)、预糊化淀粉(Colorcon LTD、Rettenmaier & Söhne (JRS),德国)、预糊化淀粉(Colorcon LTD.,英国)、Kollidone SR(巴斯夫,德国)、Croscarmellose sodium(J. Rettenmaier & Söhne(JRS),德国)、无水柠檬酸(Scharlau)、十二烷基硫酸钠(巴斯夫,德国)、Aerosil 200 vv Pharma(赢创工业股份公司,德国)、硬脂富马酸钠(J. Rettenmaier & Söhne(JRS),德国)。Rettenmaier & Söhne (JRS),德国)、硬脂酸钙(FACI,意大利)、薄膜涂层 VIVACOAT® PA-1P-000(J. Rettenmaier & Söhne (JRS),德国)。此外,还使用了 Y 型混料机("AZT FARMA K.B.",俄罗斯)、辊式压片机 LGC100(北京吉隆利自动化技术有限公司,中国)、旋转压片机 PG16G(北京吉隆利自动化技术有限公司,中国)、片剂包衣系统 VIVACOAT® PA-1P000 (J. Rettenaier & Sööne (JRS),德国)等设备、Ltd,中国)、片剂包衣系统 Labcoat™ M(O'Hara Technologies lnc,加拿大)、电离空气枪 Simco Cobra(SimcoIon,荷兰)、流动性测试仪 ERWEKA GT(ERWEKA GmbH,德国)、粉末密度测试仪 ERWEKA SVM 122(ERWEKA GmbH,德国)、振动筛 CISA RP 200N(CISA Cedaceria Industrial S.L、西班牙)、片剂硬度、厚度和高度测试仪 SOTAX HT 10(SOTAX AG,瑞士)、溶出度测试仪 DT 626/1000HH(ERWEKA GmbH,德国)和崩解度测试仪 ZT321(ERWEKA GmbH,德国)。在一系列实验中,通过直接压片和辊压法获得了片芯和薄膜衣片。实验发现,与直接压片法相比,在类似配方的片剂中,辊压技术的崩解和溶解时间更慢。在药物开发过程中,在规划活性成分的释放速度时应考虑到这一事实。实验结果表明,某种技术的使用与其对片剂崩解和溶解时间等质量指标的影响之间存在直接关系。实验还发现,干法制粒技术能提供技术上更合适的片剂质量。
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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