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Authors Li F, Zheng X, Bao YC, Chen T, Zeng J, Xu XL, Yan C, Feng LL
Received 5 July 2018
Accepted for publication 15 October 2018
Published 24 December 2018 Volume 2019:13 Pages 141—151
DOI https://doi.org/10.2147/DDDT.S179266
Checked for plagiarism Yes
Review by Single-blind
Peer reviewers approved by Dr Colin Mak
Peer reviewer comments 2
Editor who approved publication: Dr Tuo Deng
Purpose: Fenofibrate and
statin combination therapy is highly recommended by the current clinical
guidelines for treatment of mixed dyslipidemia. In this study, an innovative
delayed-release preparation of fenofibrate was designed to reduce the risk of
muscle toxicity, caused by simultaneous administration of this combination
therapy, by altering the pharmacokinetic profile of fenofibrate, as well as to
improve the oral bioavailability of the modified-release formulation.
Methods: Micronized
fenofibrate was used to prepare drug-loaded cores via a powder layering process
before multiparticulate pellet coating. Different coating formulations
(Eudragit® RS PO/E100, Eudragit® RS PO/RL
PO, Eudragit® NE30D/HPMC, and EC/HPMC) were screened,
and their in vitro release was compared with the commercial sustained-release
pellets Lipilfen®. Two optimized formulations were evaluated in
beagle dogs using two commercial preparations of fenofibrate (the
immediate-release preparation Lipanthyl® and the
sustained-release pellets Lipilfen®) as
references.
Results: The in vivo
release of fenofibrate from R1 and R2 selected from in vitro tests exhibited a
lag phase, and then rapid and complete drug release. The relative
bioavailabilities of R1 and R2 were 100.4% and 201.1%, respectively, which were
higher than that of Lipilfen® (67.2%).
Conclusion: The modified
fenofibrate pellets developed showed enhanced bioavailability and
delayed-release properties. They have the potential to improve safety and
compliance when co-administrated with statins. This is the first report of a
delayed-release fenofibrate preparation.
Keywords: fenofibrate,
modified-release pellets, coated multiparticulate pellet, pharmacokinetics, in
vivo studies
