A Phase I, Open-Label, Mass Balance Study of [C]-Iberdomide in Healthy Subjects.

Eur J Drug Metab Pharmacokinet

Clinical Pharmacology, Pharmacometrics, Disposition and Bioanalysis, Bristol Myers Squibb, Princeton, NJ, USA.

Published: May 2024

AI Article Synopsis

  • Iberdomide is a new drug being tested for blood cancers, and a study was performed to understand how it's broken down and eliminated from the body after a single dose.
  • In the study involving six healthy participants, most of the drug was found in urine (45.9%) and feces (42.6%), with the unchanged drug and its metabolites accounting for the majority of what was excreted.
  • The results showed that iberdomide mainly transforms through oxidation and hydrolysis in the body, with the drug itself being the most significant component found in the bloodstream.

Article Abstract

Background: Iberdomide is a novel potent cereblon modulator (CELMoD) agent, which is currently under clinical development for hematological malignancies. A human mass balance study was conducted to characterize the biotransformation and excretion pathways of iberdomide.

Method: After a single dose of radiolabelled [C]-iberdomide (1 mg) in six healthy subjects. Blood, urine, and fecal samples were collected for pharmacokinetics, mass balance, and clinical laboratory assessments.

Results: Results showed that a single oral dose of 1 mg iberdomide was generally well tolerated in healthy subjects. The recovery of [C]-iberdomide-derived radioactivity in humans was 45.9% in urine and 42.6% in feces. Based on exposure (area under the concentration-time curve [AUC]), iberdomide and M12 (metabolites) accounted for approximately 59% and 14% of circulating total radioactivity (TRA) exposure, respectively. Of the 88.5% TRA excreted, approximately 27% was excreted as unchanged iberdomide and 62% as metabolites, with similar amounts of excreted metabolites in the urine (16%) and feces (11%).

Conclusion: Biotransformation of iberdomide in humans included multiple oxidations of the morpholino moiety as well as glutarimide ring hydrolysis of parent and oxidized metabolites and a combination of these pathways. Iberdomide was the predominant component in human plasma, with metabolite M12 being the most prominent circulating metabolite. In excreta, similar iberdomide-derived radioactivity was found in urine and feces.

Trial Registration Number: NCT03294603.

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Source
http://dx.doi.org/10.1007/s13318-024-00886-4DOI Listing

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