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首页> 外文期刊>Pharmaceutical development and technology >Film coated tablets (ColoPulse technology) for targeted delivery in the lower intestinal tract: influence of the core composition on release characteristics.
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Film coated tablets (ColoPulse technology) for targeted delivery in the lower intestinal tract: influence of the core composition on release characteristics.

机译:薄膜包衣片剂(ColoPulse技术),可在下肠道靶向递送:核心成分对释放特性的影响。

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摘要

The design of a film coating technology which allows a tablet to deliver the drug in the ileocolonic segment would offer new treatment possibilities. The objective is to develop a platform technology that is suitable for a broad range of drug compounds. We developed a coated tablet with a delayed, pulsatile release profile based on a pH-sensitive coating technology (ColoPulse). The production process was validated, and the effect of core composition on the in vitro release and water uptake investigated. The release profile of the standard tablet core composition, based on the use of cellulose as a filler, was independent of the coat thickness in a range of 9.0-13.2?mg/cm(2). The release profile of a coated tablet was strongly influenced when cellulose was partly replaced by the model substance glucose (loss of sigmoidal release), citric acid (stabilization), sodium bicarbonate (destabilization) or sodium benzoate (destabilization). The film coating takes up water when below the pH-threshold. However, this did not cause early disintegration of the coating. The ColoPulse technology is successfully applied on tablets. The in vitro release characteristics of the coated tablets are influenced by the composition of the core.
机译:薄膜包衣技术的设计允许片剂将药物递送至回肠结肠部分,这将提供新的治疗可能性。目的是开发一种适用于多种药物化合物的平台技术。我们基于pH敏感的包衣技术(ColoPulse)开发了具有延迟,脉冲释放特性的包衣片剂。验证了生产过程,并研究了核心成分对体外释放和水分吸收的影响。基于使用纤维素作为填充剂的标准片剂核心组合物的释放曲线与涂层厚度在9.0-13.2?mg / cm(2)范围内无关。当纤维素被模型物质葡萄糖(S型释放损失),柠檬酸(稳定化),碳酸氢钠(去稳定化)或苯甲酸钠(去稳定化)部分替代时,包衣片剂的释放特性受到很大影响。当低于pH阈值时,薄膜涂层会吸收水。但是,这并没有引起涂层的早期崩解。 ColoPulse技术已成功应用于平板电脑。包衣片剂的体外释放特性受芯的组成影响。

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