Pharmacokinetic study of osilodrostat and identification of mono‐hydroxylated metabolite in equine plasma for the purpose of doping control

Ishii, Hideaki; Ishikawa, Yuhiro; Mizobe, Fumiaki; Nomura, Motoi; Yamanaka, Takashi; Tanabe, Sohei; Nagata, Shun‐ichi; Yamada, Masayuki; Leung, Gary Ngai‐Wa

doi:10.1002/rcm.9695

Rapid Comm Mass Spectrometry

2024

DOI: 10.1002/rcm.9695

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Pharmacokinetic study of osilodrostat and identification of mono‐hydroxylated metabolite in equine plasma for the purpose of doping control

Hideaki Ishii,

Yuhiro Ishikawa,

Fumiaki Mizobe

et al.

Abstract: RationaleOsilodrostat is an inhibitor of 11‐beta‐hydroxylase (CYP11B) and is used for the treatment of Cushing's disease but also categorized as an anabolic agent. The use of osilodrostat is prohibited in horseracing and equestrian sports. To the best of our knowledge, this is the first metabolic study of osilodrostat in equine plasma.MethodsPotential metabolites of osilodrostat were identified by differential analysis using data acquired from pre‐ and post‐administration plasma samples after protein precipita… Show more

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2024

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Cited by 3 publications

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Quantification of osilodrostat in horse urine using LC/ESI–HRMS to establish an elimination profile for doping control

Ishii,

Shigematsu,

Takemoto

et al. 2024

Bioanalysis

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Quantification of osilodrostat in horse urine using LC/ESI–HRMS to establish an elimination profile for doping control

Ishii,

Shigematsu,

Takemoto

et al. 2024

Bioanalysis

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Metabolic Pathway of Osilodrostat in Equine Urine Established through High-resolution Mass Spectrometric Characterization for Doping Control

Ishii,

Shigematsu,

Takemoto

et al. 2024

CDM

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Objective: Osilodrostat, used to treat Cushing's disease, exhibits an anabolic effect, leading to its classification as a prohibited substance in horseracing and equestrian sports. This study reports the characterization of osilodrostat metabolites in horse urine and elucidates its metabolic pathways for the first time for doping control purposes. Methods: Osilodrostat was administered nasoesophageally to four thoroughbreds (one gelding and three mares) at a dose of 50 mg each. Potential metabolites were extensively screened via our developed generic approach employing differential analysis to identify metabolites. Specifically, high-resolution mass spectral data were compared between pre- and post-administration samples on the basis of criteria of fold-changes of peak areas and their P values. Potential metabolite candidates were further identified through mass spectral interpretations using product ion scan data. Results: A total of 37 metabolites were identified after comprehensive analysis. Osilodrostat was predominantly metabolized into a mono-hydroxylated form M1c (~40%) alongside osilodrostat glucuronide M2 (~17%). Given their longest detection time (2 weeks after administration) and the identification of several conjugates of osilodrostat and M1c, including a novel conjugate of riburonic acid, we recommend monitoring both osilodrostat and M1c after hydrolysis during the screening stage. However, only osilodrostat can be used for confirmation because of the availability of a reference material. Conclusion: It is advisable to screen for both osilodrostat and its mono-hydroxylated metabolite M1c to effectively monitor horse urine for the potential misuse or abuse of osilodrostat. For suspicious samples, confirmation of osilodrostat using its reference material is required.

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Determination of Mefuparib in Rat Plasma and its Application to Pharmacokinetics by a Simple and Rapid UPLC-MS/MS

Chen,

Lin,

Jiang

et al. 2024

CPA

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Objectives: Mefuparib (CVL218) is a second-generation inhibitor of poly-ADP-ribose polymerase (PARP) that is used to treat cancer. In this work, CVL218 in the plasma of rats administered orally and intravenously was measured using UPLC-MS/MS. Methods: Six rats received CVL218 (3 mg/kg) orally (po), and six more rats received CVL218 (1 mg/kg) intravenously (iv). Over the range of 0.9–450 ng/mL, a standard curve representing known concentrations of CVL218 in rat plasma was produced by UPLC-MS/MS. The US Food and Drug Administration's (FDA) guidelines were followed in developing the validation method. Result: In rat plasma, accuracy ranged from 90% to 112%, but its intra- and inter-day precision was less than 15%. Furthermore, the recovery was higher than 87%, and the matrix effect varied from 102% to 113%. For intravenous and oral administration, the AUC(0-t) were 227.5 ±21.6 and 217.0 ±15.5 ng/mL·h, respectively, and the bioavailability was 31.8%. The half-life (t1/2) for oral and intravenous administration was discovered to be. 1.6 ±0.7 h and 1.7 ±0.3 h, respectively. Conclusion: The developed UPLC-MS/MS method was successfully to determinate CVL218 in rat plasma following oral and intravenous administration.

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Pharmacokinetic study of osilodrostat and identification of mono‐hydroxylated metabolite in equine plasma for the purpose of doping control

Cited by 3 publications

References 21 publications

Quantification of osilodrostat in horse urine using LC/ESI–HRMS to establish an elimination profile for doping control

Quantification of osilodrostat in horse urine using LC/ESI–HRMS to establish an elimination profile for doping control

Metabolic Pathway of Osilodrostat in Equine Urine Established through High-resolution Mass Spectrometric Characterization for Doping Control

Determination of Mefuparib in Rat Plasma and its Application to Pharmacokinetics by a Simple and Rapid UPLC-MS/MS

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