Literature DB >> 29735753

Metabolism and Disposition of Siponimod, a Novel Selective S1P1/S1P5 Agonist, in Healthy Volunteers and In Vitro Identification of Human Cytochrome P450 Enzymes Involved in Its Oxidative Metabolism.

Ulrike Glaenzel1, Yi Jin2, Robert Nufer2, Wenkui Li2, Kirsten Schroer2, Sylvie Adam-Stitah2, Sjoerd Peter van Marle2, Eric Legangneux2, Hubert Borell2, Alexander D James2, Axel Meissner2, Gian Camenisch2, Anne Gardin2.   

Abstract

Siponimod, a next-generation selective sphingosine-1-phosphate receptor modulator, is currently being investigated for the treatment of secondary progressive multiple sclerosis. We investigated the absorption, distribution, metabolism, and excretion (ADME) of a single 10-mg oral dose of [14C]siponimod in four healthy men. Mass balance, blood and plasma radioactivity, and plasma siponimod concentrations were measured. Metabolite profiles were determined in plasma, urine, and feces. Metabolite structures were elucidated using mass spectrometry and comparison with reference compounds. Unchanged siponimod accounted for 57% of the total plasma radioactivity (area under the concentration-time curve), indicating substantial exposure to metabolites. Siponimod showed medium to slow absorption (median Tmax: 4 hours) and moderate distribution (Vz/F: 291 l). Siponimod was mainly cleared through biotransformation, predominantly by oxidative metabolism. The mean apparent elimination half-life of siponimod in plasma was 56.6 hours. Siponimod was excreted mostly in feces in the form of oxidative metabolites. The excretion of radioactivity was close to complete after 13 days. Based on the metabolite patterns, a phase II metabolite (M3) formed by glucuronidation of hydroxylated siponimod was the main circulating metabolite in plasma. However, in subsequent mouse ADME and clinical pharmacokinetic studies, a long-lived nonpolar metabolite (M17, cholesterol ester of siponimod) was identified as the most prominent systemic metabolite. We further conducted in vitro experiments to investigate the enzymes responsible for the oxidative metabolism of siponimod. The selective inhibitor and recombinant enzyme results identified cytochrome P450 2C9 (CYP2C9) as the predominant contributor to the human liver microsomal biotransformation of siponimod, with minor contributions from CYP3A4 and other cytochrome P450 enzymes.
Copyright © 2018 The Author(s).

Entities:  

Mesh:

Substances:

Year:  2018        PMID: 29735753     DOI: 10.1124/dmd.117.079574

Source DB:  PubMed          Journal:  Drug Metab Dispos        ISSN: 0090-9556            Impact factor:   3.922


  13 in total

1.  Siponimod pharmacokinetics, safety, and tolerability in combination with the potent CYP3A4 inhibitor itraconazole in healthy subjects with different CYP2C9 genotypes.

Authors:  Anne Gardin; Kasra Shakeri-Nejad; Andrea Feller; Felix Huth; Srikanth Neelakantham; Swati Dumitras
Journal:  Eur J Clin Pharmacol       Date:  2019-08-07       Impact factor: 2.953

2.  Direct Carbon Isotope Exchange through Decarboxylative Carboxylation.

Authors:  Cian Kingston; Michael A Wallace; Alban J Allentoff; Justine N deGruyter; Jason S Chen; Sharon X Gong; Samuel Bonacorsi; Phil S Baran
Journal:  J Am Chem Soc       Date:  2019-01-03       Impact factor: 15.419

3.  Siponimod pharmacokinetics, safety, and tolerability in combination with rifampin, a CYP2C9/3A4 inducer, in healthy subjects.

Authors:  Anne Gardin; Cathy Gray; Srikanth Neelakantham; Felix Huth; Antonia M Davidson; Swati Dumitras; Eric Legangneux; Kasra Shakeri-Nejad
Journal:  Eur J Clin Pharmacol       Date:  2018-08-13       Impact factor: 2.953

Review 4.  Progressive multiple sclerosis: latest therapeutic developments and future directions.

Authors:  Simon Faissner; Ralf Gold
Journal:  Ther Adv Neurol Disord       Date:  2019-09-25       Impact factor: 6.570

5.  Prediction of the Impact of Cytochrome P450 2C9 Genotypes on the Drug-Drug Interaction Potential of Siponimod With Physiologically-Based Pharmacokinetic Modeling: A Comprehensive Approach for Drug Label Recommendations.

Authors:  Felix Huth; Anne Gardin; Kenichi Umehara; Handan He
Journal:  Clin Pharmacol Ther       Date:  2019-08-11       Impact factor: 6.875

6.  Pharmacokinetics and Metabolite Profiling of Trepibutone in Rats Using Ultra-High Performance Liquid Chromatography Combined With Hybrid Quadrupole-Orbitrap and Triple Quadrupole Mass Spectrometers.

Authors:  Zhi Sun; Jie Yang; Liwei Liu; Yanyan Xu; Lin Zhou; Qingquan Jia; Yingying Shi; Xiangyu Du; Jian Kang; Lihua Zuo
Journal:  Front Pharmacol       Date:  2019-11-04       Impact factor: 5.810

Review 7.  Sphingosine-1-Phosphate Receptor Modulators and Oligodendroglial Cells: Beyond Immunomodulation.

Authors:  Alessandra Roggeri; Melissa Schepers; Assia Tiane; Ben Rombaut; Lieve van Veggel; Niels Hellings; Jos Prickaerts; Anna Pittaluga; Tim Vanmierlo
Journal:  Int J Mol Sci       Date:  2020-10-13       Impact factor: 5.923

Review 8.  Abuse and dependence potential of sphingosine-1-phosphate (S1P) receptor modulators used in the treatment of multiple sclerosis: a review of literature and public data.

Authors:  Kerri A Schoedel; Carine Kolly; Anne Gardin; Srikanth Neelakantham; Kasra Shakeri-Nejad
Journal:  Psychopharmacology (Berl)       Date:  2021-11-13       Impact factor: 4.530

9.  Effect of Fluconazole Coadministration and CYP2C9 Genetic Polymorphism on Siponimod Pharmacokinetics in Healthy Subjects.

Authors:  Anne Gardin; Mike Ufer; Eric Legangneux; Gianluca Rossato; Yi Jin; Zhenzhong Su; Parasar Pal; Wenkui Li; Kasra Shakeri-Nejad
Journal:  Clin Pharmacokinet       Date:  2019-03       Impact factor: 6.447

10.  Siponimod: A Review in Secondary Progressive Multiple Sclerosis.

Authors:  Lesley J Scott
Journal:  CNS Drugs       Date:  2020-10-27       Impact factor: 5.749
View more

北京卡尤迪生物科技股份有限公司 © 2022-2023.