In Vitro Lipolysis Data Does Not Adequately Predict the In Vivo Performance of Lipid-Based Drug Delivery Systems Containing Fenofibrate

被引:0
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作者
Nicky Thomas
Katharina Richter
Thomas B. Pedersen
René Holm
Anette Müllertz
Thomas Rades
机构
[1] University of Copenhagen,Department of Pharmacy, Faculty of Health and Medical Sciences
[2] University of South Australia,Ian Wark Research Institute
[3] Biologics and Pharmaceutical Science,Bioneer:FARMA, Danish Drug Development Center, Department of Pharmacy, Faculty of Health and Medical Sciences
[4] University of Copenhagen,undefined
来源
The AAPS Journal | 2014年 / 16卷
关键词
ipolysis; /; correlation; lipids; SNEDDS suspensions; super-SNEDDS; supersaturation;
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学科分类号
摘要
The present study investigated the utility of in vitro lipolysis performance indicators drug solubilization and maximum supersaturation ratio (SRM) for their predictive use for the in vivo performance in a minipig model. The commercial Lipanthyl formulation and a series of LbDDS based on identical self-nanoemulsifying drug delivery systems (SNEDDS) containing 200 mg of fenofibrate, either dissolved or suspended, were subjected to combined gastric (pH 2) and intestinal (pH 6.5) in vitro lipolysis. Based on the solubilization profiles and SRM the rank-order SNEDDS (75% drug load) > super-SNEDDS (150% drug load, dissolved) = SNEDDS suspension (150% drug load, partially suspended) > Lipanthyl was established, with an increased likelihood of drug precipitation above SRM > 3. The in vitro performance, however, was not reproduced in vivo in a minipig model as the mean plasma concentration over time curves of all LbDDS were comparable, independent of the initial physical state of the drug. There was no correlation between the area under the solubilization-time curves (AUCin vitro) of the intestinal step and the AUCin vivo. The study suggests careful interpretation of in vitro performance criteria and revision of LbDDS optimization towards increased solubilization.
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页码:539 / 549
页数:10
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