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Cited 2 time in webofscience Cited 1 time in scopus
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A mechanism-based pharmacokinetic model of fenofibrate for explaining increased drug absorption after food consumption

Authors
Back, Hyun-moonSong, ByungjeongPradhan, SudeepChae, Jung-wooHan, NayoungKang, WonkuChang, Min JungZheng, JiaoKwon, Kwang-ilKarlsson, Mats O.Yun, Hwi-yeol
Issue Date
25-Jan-2018
Publisher
BIOMED CENTRAL LTD
Keywords
Food effect; Gastrointestinal system; Fenofibrate; NONMEM; Drug absorption
Citation
BMC PHARMACOLOGY & TOXICOLOGY, v.19, no.1
Journal Title
BMC PHARMACOLOGY & TOXICOLOGY
Volume
19
Number
1
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/1304
DOI
10.1186/s40360-018-0194-5
ISSN
2050-6511
2050-6511
Abstract
Background: Oral administration of drugs is convenient and shows good compliance but it can be affected by many factors in the gastrointestinal (GI) system. Consumption of food is one of the major factors affecting the GI system and consequently the absorption of drugs. The aim of this study was to develop a mechanistic GI absorption model for explaining the effect of food on fenofibrate pharmacokinetics (PK), focusing on the food type and calorie content. Methods: Clinical data from a fenofibrate PK study involving three different conditions (fasting, standard meals and high-fat meals) were used. The model was developed by nonlinear mixed effect modeling method. Both linear and nonlinear effects were evaluated to explain the impact of food intake on drug absorption. Similarly, to explain changes in gastric emptying time for the drug due to food effects was evaluated. Results: The gastric emptying rate increased by 61.7% during the first 6.94 h after food consumption. Increased calories in the duodenum increased the absorption rate constant of the drug in fed conditions (standard meal = 16.5%, high-fat meal = 21.8%) compared with fasted condition. The final model displayed good prediction power and precision. Conclusions: A mechanistic GI absorption model for quantitatively evaluating the effects of food on fenofibrate absorption was successfully developed, and acceptable parameters were obtained. The mechanism-based PK model of fenofibrate can quantify the effects of food on drug absorption by food type and calorie content.
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