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Investigation of the absolute bioavailability and human mass balance of navoximod, a novel IDO1 inhibitor.

Shuguang MaJulia SuchomelEvelyn YanezEdward YostXiaorong LiangRui ZhuHoa LeNicholas SiebersLori JoasRoland MorleyStephanie Royer-JooAndrea PirzkallLaurent SalphatiJoseph A WareKari M Morrissey
Published in: British journal of clinical pharmacology (2019)
Navoximod was well tolerated, quickly absorbed and showed moderate bioavailability, with minimal recovery of the dose as unchanged parent in the urine and faeces. Metabolism was identified as the primary route of clearance and navoximod glucuronide (M28) was the most abundant metabolite in circulation with all other metabolites accounting for <10% of drug-related exposure.
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