Absorption, distribution, metabolism and excretion of gemigliptin, a novel dipeptidyl peptidase IV inhibitor, in rats

Authors
Kim, YoonKim, UnyongKim, In SookLee, Sung-HackLee, JaeickKim, Dong-HyunYoo, Hye Hyun
Issue Date
2014-07
Publisher
INFORMA HEALTHCARE
Citation
XENOBIOTICA, v.44, no.7, pp.627 - 634
Abstract
1. The absorption, distribution, metabolism and excretion of a novel dipeptidyl peptidase IV inhibitor, gemigliptin, were examined following single oral administration of C-14-labeled gemigliptin to rats. 2. The C-14-labeled gemigliptin was rapidly absorbed after oral administration, and its bioavailability was 95.2% (by total radioactivity). Distribution to specific tissues other than the digestive organs was not observed. Within 7 days after oral administration, 43.6% of the administered dose was excreted via urine and 41.2% was excreted via feces. Biliary excretion of the radioactivity was about 17.7% for the first 24 h. After oral administration of gemigliptin to rats, the in vivo metabolism of gemigliptin was investigated with bile, urine, feces, plasma and liver samples. 3. The major metabolic pathway was hydroxylation, and the major circulating metabolites were a dehydrated metabolite (LC15-0516) and hydroxylated metabolites (LC15-0635 and LC15-0636).
Keywords
DOUBLE-BLIND; PHARMACOKINETICS; LC15-0444; PHARMACODYNAMICS; MULTICENTER; VOLUNTEERS; EFFICACY; SAFETY; TRIAL; DOUBLE-BLIND; PHARMACOKINETICS; LC15-0444; PHARMACODYNAMICS; MULTICENTER; VOLUNTEERS; EFFICACY; SAFETY; TRIAL; Absorption; distribution; excretion; gemigliptin; metabolism
ISSN
0049-8254
URI
https://pubs.kist.re.kr/handle/201004/126663
DOI
10.3109/00498254.2013.873156
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KIST Article > 2014
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