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Formulation and in vitro evaluation of theophylline matrix tablets prepared by direct compression: Effect of polymer blends

机译:直接压制茶碱基质片剂的配制和体外评价:聚合物共混物的作用

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摘要

The deformation mechanism of pharmaceutical powders, used in formulating directly compressed matrix tablets, affects the characteristics of the formed tablets. Three polymers of different deformation mechanisms were tested for their impact on theophylline directly compressed tablets namely Kollidon SR (KL SR, plastic deformation), Ethylcellulose (EC, elastic deformation) and Carnauba wax (CW, brittle deformation) at different compression forces. However, tablets based mainly on KL SR, the plastically deformed polymer (TN1) exhibited the highest hardness values compared to the other formulae which are based on either blends of KL SR with CW, the very brittle deformed polymer. The upper detected force for TN formulae and the lower punch force were found to dependent mainly on the powder deformation. This difference is attributed to the work done during the compression phase as well as the work lost during the decompression phase. Furthermore, the release profiles of TN from formulae TN2 and TN4 that are based on the composition (2KL SR:1EC) and (1KL SR:2EC), respectively, were consistent with different deformation mechanisms of KL SR and EC and on the physicochemical properties like the water absorptive capacity of EC. Upon increasing the weight ratio of KL SR (TN2), the release rate was greatly retarded (39.4%, 37.1%, 35.0% and 33.6% released after 8 h at 5, 10, 15 and 20 kN.
机译:用于配制直接压制的基质片剂的药物粉末的变形机理影响所形成的片剂的特性。测试了三种不同变形机制的聚合物对茶碱直接压片的影响,分别为Kollidon SR(KL SR,塑性变形),乙基纤维素(EC,弹性变形)和巴西棕榈蜡(CW,脆性变形)。但是,与其他基于KL SR与CW(非常脆的变形聚合物)的共混物的配方相比,主要基于KL SR塑性变形聚合物(TN1)的片剂显示出最高的硬度值。发现TN公式的较高检测力和较低冲模力主要取决于粉末变形。这种差异归因于在压缩阶段完成的功以及在减压阶段丢失的功。此外,分别基于组成(2KL SR:1EC)和(1KL SR:2EC)的配方TN2和TN4的TN释放曲线与KL SR和EC的不同变形机理以及理化性质一致就像EC的吸水能力增加KL SR(TN2)的重量比后,释放速率大大降低(在5、10、15和20 kN下8小时后释放的分别为39.4%,37.1%,35.0%和33.6%。

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