Received for publication August 16, 2006.
Revised October 20, 2006.
Accepted for publication October 20, 2006.
COMPARATIVE METABOLISM OF RADIOLABELED MURAGLITAZAR IN ANIMALS AND HUMANS BY QUANTITATIVE AND QUALITATIVE METABOLITE PROFILING
Donglu Zhang 1*,
Lifei Wang 2,
Nirmala Raghavan 1,
Haiying Zhang 1,
Wenying Li 1,
Peter T Cheng 1,
Ming Yao 1,
Litao Zhang 1,
Mingshe Zhu 1,
Samuel Bonacorsi 1,
Suresh Yeola 1,
James Mitroka 1,
Narayanan Hariharan 1,
Vinayak Hosagrahara 1,
Gamini Chandrasena 1,
Wen Chyi Shyu 1,
W Griffith Humphreys 1
1 Bristol-Myers Squibb
2 Bristol-Myers squibb
* Address correspondence to: E-mail: donglu.zhang{at}bms.com
Abstract
Muraglitazar (Pargluva), a dual alpha/gamma PPAR activator, has both glucose and lipid lowering effects in animal models and in patients with diabetes. This study describes the in vivo and in vitro comparative metabolism of [14C]muraglitazar in rats, dogs, monkeys, and humans by quantitative and qualitative metabolite profiling. Metabolite identification and quantification methods used in these studies included LC/MS, LC/MS/MS, LC/radiodetection, LC/UV, and a newly described mass defect filtering technique in conjunction with high resolution MS. Following oral administration of [14C]muraglitazar, absorption was rapid in all species, reaching a concentration peak for parent and total radioactivity in plasma within 1 hour. The most abundant component in plasma at all times in all species was the parent drug, and no metabolite was present in greater than 2.5% of the muraglitazar concentrations at 1 hour post dose in rats, dogs, and humans. All metabolites observed in humans plasma were also present in rats, dogs, or monkeys. Urinary excretion of radioactivity was low (<5% of the dose) in all intact species and the primary route of elimination was via biliary excretion in rats, monkeys, and humans. Based on recovered doses in urine and bile, muraglitazar showed a very good absorption in rats, monkeys, and humans. The major drug-related components in bile of rats, monkeys, and humans were glucuronides of muraglitazar and its oxidative metabolites. The parent compound was a minor component in bile, suggesting extensive metabolism of the drug. In contrast, the parent drug and oxidative metabolites were the major components in feces and no glucuronide conjugates were found, suggesting that glucuronide metabolites were excreted in bile and hydrolyzed in the gastrointestinal tract. The metabolites of muraglitazar resulted from both glucuronidation and oxidation. The metabolites in general had greatly reduced activity as PPAR
/
activators relative to muraglitazar. In conclusion, muraglitazar was rapidly absorbed, extensively metabolized through glucuronidation and oxidation, and mainly eliminated in the feces via biliary excretion of glucuronide metabolites in all species studied. Disposition and metabolic pathways were qualitatively similar in rats, dogs, monkeys, and humans.
Key words:
analytical chemistry, biliary excretion, drug disposition, hepatocytes, HPLC
![[Feedback]](/icons/banner/feedbackACT.gif){kind=icon}
![[For Subscribers]](/icons/banner/subscriberACT.gif){kind=icon}
![[Archive]](/icons/banner/archiveACT.gif){kind=icon}
![[Search]](/icons/banner/searchACT.gif){kind=icon}
