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Food Effects on Oral Drug Absorption: Application of Physiologically-Based Pharmacokinetic Modeling as a Predictive Tool

机译:对口腔吸毒的食物作用:基于生理学药代理建模的应用作为预测工具

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The bioavailability of an orally administered small molecule is often dictated by drug-specific physicochemical characteristics and is influenced by many biological processes. For example, in fed or fasted conditions, the transit time within the gastrointestinal tract can vary, confounding the ability to predict the oral absorption. As such, the effects of food on the pharmacokinetics of compounds in the various biopharmaceutics classification system (BCS) classes need to be assessed. The consumption of food leads to physiological changes, including fluctuations in the gastric and intestinal pH, a delay in gastric emptying, an increased bile secretion, and an increased splanchnic and hepatic blood flow. Despite the significant impact of a drug’s absorption and dissolution, food effects have not been fully studied and are often overlooked. Physiologically-based pharmacokinetic (PBPK) models can be used to mechanistically simulate a compound’s pharmacokinetics under fed or fasted conditions, while integrating drug properties such as solubility and permeability. This review discusses the PBPK models published in the literature predicting the food effects, the models’ strengths and shortcomings, as well as future steps to mitigate the current knowledge gap. We observed gaps in knowledge which limits the ability of PBPK models to predict the negative food effects and food effects in the pediatric population. Overall, the further development of PBPK models to predict food effects will provide a mechanistic basis to understand a drug’s behavior in fed and fasted conditions, and will help enable the drug development process.
机译:口服给药的小分子的生物利用度通常通过药物特异性物理化学特征决定,受许多生物过程的影响。例如,在喂养或禁食条件下,胃肠道内的过渡时间可以变化,混淆预测口腔吸收的能力。因此,需要评估食物对各种生物制冷分类系统(BCS)课程中化合物的药代动力学的影响。食物的消费导致生理变化,包括胃和肠pH的波动,胃排空的延迟,胆汁分泌增加,以及增加的脾气和肝血流量。尽管药物的吸收和溶解产生重大影响,但尚未完全研究食品效果,并且往往被忽视。基于生理学的药代动力学(PBPK)模型可用于机械地在喂养或禁食条件下模拟化合物的药代动力学,同时整合药物性质,例如溶解度和渗透性。该审查讨论了在文献中发表的PBPK模型,预测食物效果,模型的优势和缺点,以及减轻当前知识间隙的未来步骤。我们观察到知识的差距,这限制了PBPK模型预测儿科人群中的负食物效果和食物效果的能力。总体而言,PBPK模型的进一步发展预测粮食效果将为喂养和禁食条件中了解药物的行为,并将有助于提高药物开发过程。

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