Linking the Gastrointestinal Behavior of Ibuprofen with the Systemic Exposure between and within Humans-Part 1: Fasted State Conditions

Marival Bermejo; Paulo Paixão; Bart Hens; Yasuhiro Tsume; Mark J Koenigsknecht; Jason R Baker; William L Hasler; Robert Lionberger; Jianghong Fan; Joseph Dickens; Kerby Shedden; Bo Wen; Jeffrey Wysocki; Raimar Löbenberg; Allen Lee; Ann Frances; Gregory E Amidon; Alex Yu; Niloufar Salehi; Arjang Talattof; Gail Benninghoff; Duxin Sun; Gislaine Kuminek; Katie L Cavanagh; Naír Rodríguez-Hornedo; Gordon L Amidon

doi:10.1021/acs.molpharmaceut.8b00515

Linking the Gastrointestinal Behavior of Ibuprofen with the Systemic Exposure between and within Humans-Part 1: Fasted State Conditions

Mol Pharm. 2018 Dec 3;15(12):5454-5467. doi: 10.1021/acs.molpharmaceut.8b00515. Epub 2018 Nov 12.

Authors

Marival Bermejo^{1

2}, Paulo Paixão³, Bart Hens^{1

4}, Yasuhiro Tsume¹, Mark J Koenigsknecht¹, Jason R Baker, William L Hasler, Robert Lionberger⁵, Jianghong Fan⁵, Joseph Dickens, Kerby Shedden, Bo Wen¹, Jeffrey Wysocki¹, Raimar Löbenberg⁶, Allen Lee¹, Ann Frances¹, Gregory E Amidon¹, Alex Yu¹, Niloufar Salehi⁷, Arjang Talattof¹, Gail Benninghoff¹, Duxin Sun¹, Gislaine Kuminek¹, Katie L Cavanagh¹, Naír Rodríguez-Hornedo¹, Gordon L Amidon¹

Affiliations

¹ Department of Pharmaceutical Sciences, College of Pharmacy , University of Michigan , 428 Church Street , Ann Arbor , Michigan 48109-1065 , United States.
² Department of Engineering, Pharmacy Section , Miguel Hernandez University , San Juan de Alicante, 03550 Alicante , Spain.
³ Research Institute for Medicines (iMed.ULisboa), Faculty of Pharmacy , Universidade de Lisboa , Avenida Professor Gama Pinto , 1649-003 Lisboa , Portugal.
⁴ Department of Pharmaceutical and Pharmacological Sciences , KU Leuven , Herestraat 49 , 3000 Leuven , Belgium.
⁵ Office of Generic Drugs, Center for Drug Evaluation and Research , U.S. Food and Drug Administration , Silver Spring , Maryland 20993 , United States.
⁶ Faculty of Pharmacy & Pharmaceutical Sciences , University of Alberta , Edmonton , Alberta , Canada T6G 2H7.
⁷ Center for the Study of Complex Systems and Department of Chemical Engineering , University of Michigan , Ann Arbor , Michigan 48109-2136 , United States.

Abstract

The goal of this project was to explore and to statistically evaluate the responsible gastrointestinal (GI) factors that are significant factors in explaining the systemic exposure of ibuprofen, between and within human subjects. In a previous study, we determined the solution and total concentrations of ibuprofen as a function of time in aspirated GI fluids, after oral administration of an 800 mg IR tablet (reference standard) of ibuprofen to 20 healthy volunteers in fasted state conditions. In addition, we determined luminal pH and motility pressure recordings that were simultaneously monitored along the GI tract. Blood samples were taken to determine ibuprofen plasma levels. In this work, an in-depth statistical and pharmacokinetic analysis was performed to explain which underlying GI variables are determining the systemic concentrations of ibuprofen between (inter-) and within (intra-) subjects. In addition, the obtained plasma profiles were deconvoluted to link the fraction absorbed with the fraction dissolved. Multiple linear regressions were performed to explain and quantitatively express the impact of underlying GI physiology on systemic exposure of the drug (in terms of plasma C_max/AUC and plasma T_max). The exploratory analysis of the correlation between plasma C_max/AUC and the time to the first phase III contractions postdose (TMMC-III) explains ∼40% of the variability in plasma C_max for all fasted state subjects. We have experimentally shown that the in vivo intestinal dissolution of ibuprofen is dependent upon physiological variables like, in this case, pH and postdose phase III contractions. For the first time, this work presents a thorough statistical analysis explaining how the GI behavior of an ionized drug can explain the systemic exposure of the drug based on the individual profiles of participating subjects. This creates a scientifically based and rational framework that emphasizes the importance of including pH and motility in a predictive in vivo dissolution methodology to forecast the in vivo performance of a drug product. Moreover, as no extensive first-pass metabolism is considered for ibuprofen, this study demonstrates how intraluminal drug behavior is reflecting the systemic exposure of a drug.

Keywords: aspiration/motility study; bioavailability; bioequivalence; ibuprofen; immediate release; in vivo dissolution; local drug concentration in the GI tract; manometry; motility; oral absorption.

Publication types

Randomized Controlled Trial
Research Support, Non-U.S. Gov't
Research Support, U.S. Gov't, P.H.S.

MeSH terms

Administration, Oral
Adult
Area Under Curve
Biological Availability
Biological Variation, Individual
Biological Variation, Population / physiology
Datasets as Topic
Drug Liberation*
Fasting / physiology*
Female
Gastrointestinal Absorption / physiology*
Gastrointestinal Tract / physiology*
Healthy Volunteers
Humans
Hydrogen-Ion Concentration
Ibuprofen / administration & dosage
Ibuprofen / pharmacokinetics*
Male
Middle Aged
Models, Biological
Solubility
Tablets
Young Adult

Substances

Tablets
Ibuprofen

Grants and funding

P30 CA046592/CA/NCI NIH HHS/United States