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Medical Plastics for Oral Dosage Forms with Drug Controlled Release

机译:用于口服剂型的医疗塑料与药物控释释放

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Conventional oral dosage forms with immediate release are associated with plasma drug levels alternating between high peaks and low troughs. Therapy is optimized by using oral dosage forms with controlled release. Usually dosage forms with drug controlled release consist of devices where the drug is dispersed through a biocompatible polymer which plays the role of a matrix, and thus the polymer plays the major role for controlling the drug release along the gastrointestinal tract. Depending on the nature of the polymer, the process of drug release is different. Two extreme cases are considered here: the one with stable polymers where the drug release is controlled by diffusion with the more simple case of constant diffusivity; the other with erodible polymers with a constant rate of erosion. As the gastrointestinal transit time is finite, the radius of spherical dosage forms is evaluated so that the time of drug delivery is 24 h. Various shapes are also considered with the same polymer and the same diffusivity or rate of erosion, by keeping the same volume and mass of drug for these dosage forms. The plasma drug level is also assessed for these two types of dosage forms. Some results of interest are obtained: for each type of polymer, the shape given to the dosage form exhibits some interest for the kinetics of drug release; the type of polymer is of prime importance, and erodible polymers are associated with a more constant plasma drug level. Thus these results take stock of the question of drug release by considering the properties of the polymer, whether it is stable with its diffusity or it is erodible with its rate of erosion. An advantage appears for the erosional polymers, since they can adhere to the gastrointestinal membrane over a time far longer than 24 h, leading to a more constant drug level in the plasma.
机译:具有即时释放的常规口腔剂型与高峰和低谷之间交替的血浆药物水平相关。通过使用具有控制释放的口服剂型进行优化治疗。通常具有药物控释释放的剂型由药物分散通过发挥基质作用的药物,因此聚合物在胃肠道控制药物释放的主要作用中。根据聚合物的性质,药物释放过程是不同的。这里考虑了两个极端情况:具有稳定聚合物的聚合物,其中药物释放通过扩散来控制恒定扩散率的更简单的情况;另一个具有恒定腐蚀速率的可蚀的聚合物。随着胃肠道传输时间是有限的,评估球形剂型的半径,使得药物递送时间为24小时。通过保持相同的体积和质量的这些剂型,还考虑各种形状和相同的聚合物和侵蚀率相同的扩散性或侵蚀速率。还评估了这两种剂型的血浆药物水平。获得了一些兴趣的结果:对于每种类型的聚合物,给予剂型的形状对药物释放的动力学表现出一些兴趣;聚合物的类型是主要的重要性,并且可蚀刻的聚合物与更恒定的血浆药物水平相关。因此,这些结果通过考虑聚合物的性质,通过其散射率稳定,呈现出药物释放问题的库存,或者它与其腐蚀速度是令人侵蚀的。侵蚀聚合物出现的优势,因为它们可以在比24小时长的时间内粘附到胃肠膜上,导致血浆中的更恒定的药物水平。

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