Estimating the variability in fraction absorbed as a paradigm for informing formulation development in early clinical drug development

Rabbie Sarit Cohen; Martin Paul D.; Flanagan Talia; Basit Abdul W.; Standing Joseph F.

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Estimating the variability in fraction absorbed as a paradigm for informing formulation development in early clinical drug development

机译：估计吸收分数的变异性，作为在早期临床药物开发中告知制剂开发的范例

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Purpose: Inter-subject variability in oral drug absorption is usually reported using bioavailability, which has the components: fraction absorbed (f(a)), fraction passing the gut wall (f(g)) and fraction escaping hepatic metabolism (f(h)). In this study, we sought to separate the absorption (f(a) (*) f(g)) and elimination (f(h)) components of bioavailability to study variability of absorption and to investigate the effect of formulations, gastric pH and food on absorption variability.

机译：目的：通常使用生物利用度来报告受试者间口服药物吸收的变异性，其组成包括：吸收的分数（f（a）），通过肠道壁的分数（f（g））和逃逸的肝代谢分数（f（h ））。在这项研究中，我们试图分离生物利用度的吸收（f（a）（*）f（g））和消除（f（h））成分，以研究吸收的变异性并研究制剂，胃液pH和食物的吸收变异性。

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《European journal of pharmaceutical sciences》 |2016年第null期|共11页
作者
Rabbie Sarit Cohen; Martin Paul D.; Flanagan Talia; Basit Abdul W.; Standing Joseph F.;
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原文格式 PDF
正文语种 eng
中图分类药学;
关键词
Inter-subject variability; Absorption; Bioavailability; Formulation; Food effect;

机译：受试者间变异;吸收;生物利用度;配方;食物效应;

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专利

1. Estimating the variability in fraction absorbed as a paradigm for informing formulation development in early clinical drug development [J] . Rabbie Sarit Cohen, Martin Paul D., Flanagan Talia, European journal of pharmaceutical sciences . 2016,第Null期

机译：估计吸收分数的变异性，作为在早期临床药物开发中告知制剂开发的范例
2. How clinical trials of myasthenia gravis can inform pre-clinical drug development [J] . Punga Anna Rostedt, Kaminski Henry J., Richman David P., Experimental Neurology . 2015,第Null期

机译：重症肌无力的临床试验如何为临床前药物开发提供信息
3. Utilizing Physiologically Based Pharmacokinetic Modeling to Inform Formulation and Clinical Development for a Compound with pH-Dependent Solubility [J] . Chung John, Alvarez-Nunez Fernando, Chow Vincent, Journal of pharmaceutical sciences. . 2015,第4期

机译：利用基于生理的药代动力学模型来指导具有pH依赖性溶解度的化合物的配制和临床开发
4. Development of Clinical Dosage Forms for a Poorly Water-Soluble Drug II: Comparative Evaluation of Solid Dispersion, Solid Microemulsion Preconcentrate and Lipid-based Formulations [C] . Rose-Marie Dannenfelser, Handan He, Ping Li, Controlled Release Society Annual Meeting and Exposition . 2007

机译：水溶性差的药物的临床剂型开发II：固体分散体，固体微乳液预浓缩物和脂质基制剂的比较评价
5. Learn & Apply Paradigm to Inform Drug Development & Optimize Clinical Therapeutics in Oncology. [D] . Mehrotra, Shailly. 2017

机译：学习和应用范例，以指导药物开发和优化肿瘤学的临床疗法。
6. How Clinical Trials of Myasthenia Gravis Can Inform Pre-Clinical Drug Development [O] . Anna Rostedt Punga, Henry J. Kaminski, David P. Richman, -1

机译：重症肌无力的临床试验如何告知临床前药物开发
7. Estimating the variability in fraction absorbed as a paradigm for informing formulation development in early clinical drug development [O] . Sarit Cohen Rabbie, Paul D. Martin, Talia Flanagan, 2016

机译：估计作为临床药物开发中的制剂发育的范式吸收的级分中的变异性

Estimating the variability in fraction absorbed as a paradigm for informing formulation development in early clinical drug development

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