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Characterization of fimasartan metabolites in human liver microsomes and human plasma

Authors
Lee, Ji-YoonChoi, Young JaeOh, Soo JinChi, Yong HaPaik, Soo HeuiLee, Ki HoJung, Jae-KyungRyu, Chang SeonKim, Kwon-BokKim, Dong-HyunYoon, Young-RanKim, Sang Kyum
Issue Date
2-Jan-2016
Publisher
TAYLOR & FRANCIS LTD
Keywords
Fimasartan; metabolic stability; metabolite identification; qualitative and quantitative analysis
Citation
XENOBIOTICA, v.46, no.1, pp.40 - 51
Indexed
SCIE
SCOPUS
Journal Title
XENOBIOTICA
Volume
46
Number
1
Start Page
40
End Page
51
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/89843
DOI
10.3109/00498254.2015.1047429
ISSN
0049-8254
Abstract
1.The metabolites of fimasartan (FMS), a new angiotensin II receptor antagonist, were characterized in human liver microsomes (HLM) and human subjects.2.We developed a method for a simultaneous quantitative and qualitative analysis using predictive multiple reaction monitoring information-dependent acquisition-enhanced product ion scanning. To characterize metabolic reactions, FMS metabolites were analyzed using quadrupole-time of flight mass spectrometer in full-scan mode.3.The structures of metabolites were confirmed by comparison of chromatographic retention times and mass spectra with those of authentic metabolite standards.4.In the cofactor-dependent microsomal metabolism study, the half-lives of FMS were 56.7, 247.9 and 53.3min in the presence of NADPH, UDPGA and NADPH+UDPGA, respectively.5.The main metabolic routes in HLM were S-oxidation, oxidative desulfuration, n-butyl hydroxylation and N-glucuronidation.6.In humans orally administered with 120mg FMS daily for 7 days, the prominent metabolites were FMS S-oxide and FMS N-glucuronide in the 0-8-h pooled plasma sample of each subject.7.This study characterizes, for the first time, the metabolites of FMS in humans to provide information for its safe use in clinical medicine.
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