| Literature DB >> 27499331 |
Jimmy Flarakos1, Yancy Du1, Helen Gu1, Lai Wang1, Heidi J Einolf1, Dung Y Chun1, Bing Zhu1, Natalia Alexander1, Adrienne Natrillo1, Imad Hanna1, Lillian Ting2, Wei Zhou1, Kiran Dole3, Haiying Sun1, Steven J Kovacs3, Daniel S Stein3, S Ken Tanaka4, Stephen Villano4, James B Mangold1.
Abstract
1. Absorption, distribution, metabolism, transport and elimination properties of omadacycline, an aminomethylcycline antibiotic, were investigated in vitro and in a study in healthy male subjects. 2. Omadacycline was metabolically stable in human liver microsomes and hepatocytes and did not inhibit or induce any of the nine cytochrome P450 or five transporters tested. Omadacycline was a substrate of P-glycoprotein, but not of the other transporters. 3. Omadacycline metabolic stability was confirmed in six healthy male subjects who received a single 300 mg oral dose of [14C]-omadacycline (36.6 μCi). Absorption was rapid with peak radioactivity (∼610 ngEq/mL) between 1-4 h in plasma or blood. The AUClast of plasma radioactivity (only quantifiable to 8 h due to low radioactivity) was 3096 ngEq h/mL and apparent terminal half-life was 11.1 h. Unchanged omadacycline reached peak plasma concentrations (∼563 ng/mL) between 1-4 h. Apparent plasma half-life was 17.6 h with biphasic elimination. Plasma exposure (AUCinf) averaged 9418 ng h/mL, with high clearance (CL/F, 32.8 L/h) and volume of distribution (Vz/F 828 L). No plasma metabolites were observed. 4. Radioactivity recovery of the administered dose in excreta was complete (>95%); renal and fecal elimination were 14.4% and 81.1%, respectively. No metabolites were observed in urine or feces, only the omadacycline C4-epimer.Entities:
Keywords: Aminomethylcycline; cytochrome P450; human; transporters
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Year: 2016 PMID: 27499331 DOI: 10.1080/00498254.2016.1213465
Source DB: PubMed Journal: Xenobiotica ISSN: 0049-8254 Impact factor: 1.908