| Literature DB >> 30417648 |
Paulo Paixão1,2, Marival Bermejo1,3, Bart Hens1,4, Yasuhiro Tsume1, Joseph Dickens, Kerby Shedden, Niloufar Salehi5, Mark J Koenigsknecht1, Jason R Baker6, William L Hasler6, Robert Lionberger7, Jianghong Fan7, Jeffrey Wysocki1, Bo Wen1, Allen Lee6, Ann Frances1, Gregory E Amidon1, Alex Yu1, Gail Benninghoff1, Raimar Löbenberg8, Arjang Talattof1, Duxin Sun1, Gordon L Amidon1.
Abstract
Exploring the intraluminal behavior of an oral drug product in the human gastrointestinal (GI) tract remains challenging. Many in vivo techniques are available to investigate the impact of GI physiology on oral drug behavior in fasting state conditions. However, little is known about the intraluminal behavior of a drug in postprandial conditions. In a previous report, we described the mean solution and total concentrations of ibuprofen after oral administration of an immediate-release (IR) tablet in fed state conditions. In parallel, blood samples were taken to assess systemic concentrations. The purpose of this work was to statistically evaluate the impact of GI physiology (e.g., pH, contractile events) within and between individuals (intra and intersubject variability) for a total of 17 healthy subjects. In addition, a pharmacokinetic (PK) analysis was performed by noncompartmental analysis, and PK parameters were correlated with underlying physiological factors (pH, time to phase III contractions postdose) and study parameters (e.g., ingested amount of calories, coadministered water). Moreover, individual plasma profiles were deconvoluted to assess the fraction absorbed as a function of time, demonstrating the link between intraluminal and systemic behavior of the drug. The results demonstrated that the in vivo dissolution of ibuprofen depends on the present gastric pH and motility events at the time of administration. Both intraluminal factors were responsible for explaining 63% of plasma Cmax variability among all individuals. For the first time, an in-depth analysis was performed on a large data set derived from an aspiration/motility study, quantifying the impact of physiology on systemic behavior of an orally administered drug product in fed state conditions. The data obtained from this study will help us to develop an in vitro biorelevant dissolution approach and optimize in silico tools in order to predict the in vivo performance of orally administered drug products, especially in fed state conditions.Entities:
Keywords: bioavailability; bioequivalence; buffer capacity; fed state; ibuprofen; immediate release; in vivo dissolution; in vivo study; local drug concentration in the GI tract; manometry; motility; oral absorption
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Year: 2018 PMID: 30417648 PMCID: PMC8859981 DOI: 10.1021/acs.molpharmaceut.8b00736
Source DB: PubMed Journal: Mol Pharm ISSN: 1543-8384 Impact factor: 4.939