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Increasing the biorelevance of simulated intestinal fluids for better predictions of drug equilibrium solubility in the fasted upper small intestine

机译:增加模拟肠液的生物相关性,以便更好地预测禁食上小肠中药物平衡的溶解度

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摘要

To date the importance of luminal species other than bile salts and phosphatidylcholine on drug equilibrium solubility in the fasted upper small intestine has been evaluated to a very limited extent. In this communication the importance of fatty acids, cholesterol, and proteins on solubility of four model lipophilic compounds was evaluated by including these components into previously proposed simulated intestinal fluids. Data were compared with ex vivo solubility data in aspirates reflecting the mean and the median luminal composition in the upper small intestine. It is concluded that estimation of solubility in aspirates reflecting the median luminal composition is better estimated when the presence of cholesterol and fatty acids is also simulated. In contrast, estimation of solubility in aspirates reflecting the mean luminal composition requires consideration of additional factors (e.g. buffer species identity, non-micellar colloidal structures, and lyso-phosphatidylcholine content).
机译:迄今为止,已经在非常有限的程度上评估了胆汁盐和磷脂酰胆碱以外的其他管腔物质对禁食上部小肠中药物平衡溶解度的重要性。在此交流中,通过将这些成分包括在先前提出的模拟肠液中,评估了脂肪酸,胆固醇和蛋白质对四种模型亲脂性化合物溶解度的重要性。将数据与吸出物中的离体溶解度数据进行比较,反映出小肠上部的平均和中位腔组成。结论是,当还模拟胆固醇和脂肪酸的存在时,可以更好地估计反映中位腔组成的抽吸物中溶解度的估计值。相反,估计反映平均管腔组成的抽吸物中的溶解度需要考虑其他因素(例如缓冲液种类,非胶束胶体结构和溶血磷脂酰胆碱含量)。

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