Pharmacokinetics and Metabolism of Ziritaxestat (GLPG1690) in Healthy Male Volunteers Following Intravenous and Oral Administration

Helmer, Eric; Willson, Ashley; Brearley, Christopher J.; Westerhof, Mark; Delage, Stephane; Shaw, Iain; Cooke, Ray; Sidhu, Sharan

doi:10.1002/cpdd.1021

Cited by 9 publications

(21 citation statements)

References 37 publications

(108 reference statements)

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“…Ziritaxestat PK parameters following the 600 mg q.d. dose were similar to those observed in previous studies in healthy male volunteers, 3,5 indicating that subjects were exposed as expected to ziritaxestat.…”

Section: Discussionsupporting

confidence: 89%

“…and oral contraceptive vs. oral contraceptive alone; however, ziritaxestat was generally well tolerated with a safety profile consistent with findings from previous studies in healthy male subjects. 3,5 Ziritaxestat PK parameters following the 600 mg q.d. dose were similar to…”

Section: Discussionmentioning

confidence: 99%

“…In vitro studies indicate that ziritaxestat is a weak inducer and inhibitor of CYP3A4. 3 Predictions based on the in vitro data indicated that ziritaxestat-mediated induction of CYP3A4 is expected to decrease exposure of a CYP3A4 probe substrate by ≤ 30%, with inhibition expected to result in a maximum increase in probe substrate metabolism of 1.5-fold. The inhibition of CYP3A4 was competitive and reversible (data on file).…”

Section: How Might This Change Clinical Pharma-cology or Translationa...mentioning

confidence: 99%

“…Laboratory tests, vital signs measurement, 12-lead electrocardiograms (ECGs), and physical examinations were performed at screening, day 1, and at follow-up (full details shown in Table S1). Ziritaxestat PKs were also evaluated as a secondary end point in this study, but as these parameters have been described in detail previously, 3,5 they will not be reported further here. Other study end points included performing an in vivo analysis of SULT1E1 and UGT1A1 inhibition by ziritaxestat.…”

Section: Articlementioning

confidence: 99%

“…Ziritaxestat (GLPG1690) is an autotaxin inhibitor that was, until recently, in development for the oral treatment of fibrotic diseases, such as idiopathic pulmonary fibrosis (phase III clinical trial registration numbers: NCT03711162 and NCT03733444) and systemic sclerosis (phase IIa clinical trial registration number: NCT03798366). In vitro studies indicate that ziritaxestat is a weak inducer and inhibitor of CYP3A4 3 . Predictions based on the in vitro data indicated that ziritaxestat‐mediated induction of CYP3A4 is expected to decrease exposure of a CYP3A4 probe substrate by ≤ 30%, with inhibition expected to result in a maximum increase in probe substrate metabolism of 1.5‐fold.…”

mentioning

confidence: 99%

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Ziritaxestat Drug–Drug Interaction with Oral Contraceptives: Role of SULT1E1 Inhibition

Helmer

Karimian

Assche

et al. 2022

Clin Pharma and Therapeutics

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In vitro signals indicate that ziritaxestat is a weak cytochrome P450 (CYP) 3A4 inhibitor and inducer. Therefore, potential drug-drug interactions (DDIs) with oral contraceptives were examined at a time when ziritaxestat was under development for treatment of fibrotic diseases. This open-label, crossover (fixed sequence) DDI study enrolled healthy, nonpregnant women aged 18-65 years (n = 15) who were using highly effective contraception, such as a nonhormonal intrauterine device, bilateral tubal occlusion, or sexual abstinence. A single dose of oral contraceptive (0.03 mg ethinyl estradiol (EE) and 3 mg drospirenone (DRSP)) was administered on days 1, 8, and 18, and ziritaxestat 600 mg once daily was administered from days 8 to 23. Co-administration resulted in a 2.8-fold and 2.4-fold increase in EE maximum plasma concentration (C max ) and area under the plasma drug concentration-time curve from time zero to infinity (AUC 0-inf ), respectively (day 18 vs. day 1). DRSP C max and AUC 0-inf increased by 1.1-fold and 1.2-fold, respectively. DRSP is a CYP3A4 substrate, meaning increased EE exposure with ziritaxestat was not due to CYP3A4 inhibition. Ziritaxestat inhibition of EE glucuronidation and sulfation was quantified by liquid chromatography with tandem mass spectrometry in day 1 and day 18 plasma samples after EE conjugate hydrolysis. The ratio of EE AUC from time of administration up to the time of the last quantifiable concentration (AUC last ) with/without hydrolysis by arylsulfatase was substantially lower on day 18 vs. day 1, suggesting ziritaxestat is a potent inhibitor of sulfation; EE glucuronidation was largely unaffected by ziritaxestat. In vitro assessment confirmed ziritaxestat is a potent inhibitor of sulfotransferase family 1E member 1 (half-maximal inhibitory concentration < 0.8 μM). These findings highlight the importance of assessing enzymes other than CYP3A4 when investigating potential DDIs with oral contraceptives.

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Section: Discussionsupporting

confidence: 89%

Section: Discussionmentioning

confidence: 99%

Section: How Might This Change Clinical Pharma-cology or Translationa...mentioning

confidence: 99%

Section: Articlementioning

confidence: 99%

mentioning

confidence: 99%

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Ziritaxestat Drug–Drug Interaction with Oral Contraceptives: Role of SULT1E1 Inhibition

Helmer

Karimian

Assche

et al. 2022

Clin Pharma and Therapeutics

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ISABELA Studies: Plasma Exposure and Target Engagement Do Not Explain the Lack of Efficacy of Ziritaxestat in Patients with Idiopathic Pulmonary Fibrosis

Taneja,

Jentsch,

Delage

et al. 2024

Clin Pharma and Therapeutics

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Autotaxin (ATX) contributes to the production of lysophosphatidic acid (LPA), which is associated with fibrosis development in idiopathic pulmonary fibrosis (IPF). The ATX inhibitor, ziritaxestat, failed to reduce decline in forced vital capacity (FVC) in patients with IPF in ISABELA 1 and 2 (NCT03711162; NCT03733444), two identically designed Phase 3 studies. In the current analysis, we evaluated pharmacokinetic and pharmacodynamic data from the pooled ISABELA studies to determine whether the lack of efficacy could be attributed to insufficient exposure and/or target engagement. Non‐linear mixed effect modeling was performed to predict ziritaxestat exposure in individual patients and describe its effect on LPA C18:2 levels. We assessed whether there was a correlation between ziritaxestat and ATX concentration and evaluated the relationship between LPA C18:2 reduction and change from baseline in FVC. Ziritaxestat exposure in patients with IPF was numerically lower in those who received ziritaxestat on top of pirfenidone than in those who received ziritaxestat on top of nintedanib or ziritaxestat alone. In most patients, LPA C18:2 reduction was comparable to that reported in healthy volunteers. ATX concentrations increased over time and correlated weakly with ziritaxestat exposure and LPA C18:2 reduction. No correlation between reduction in LPA C18:2 and change from baseline in FVC was apparent. Based on these evaluations, exposure and target engagement are not thought to have contributed to the lack of efficacy observed. We hypothesize that the lack of efficacy of ziritaxestat in the ISABELA program, despite adequate LPA reduction, could be due to the involvement of an alternative pro‐fibrotic pathway.

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Design, conduct, and interpretation of human mass balance studies and strategies for assessing metabolites-in-safety testing (MIST) in drug development

Wong

2023

Overcoming Obstacles in Drug Discovery and Development

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Pharmacokinetics and Metabolism of Ziritaxestat (GLPG1690) in Healthy Male Volunteers Following Intravenous and Oral Administration

Cited by 9 publications

References 37 publications

Ziritaxestat Drug–Drug Interaction with Oral Contraceptives: Role of SULT1E1 Inhibition

Ziritaxestat Drug–Drug Interaction with Oral Contraceptives: Role of SULT1E1 Inhibition

ISABELA Studies: Plasma Exposure and Target Engagement Do Not Explain the Lack of Efficacy of Ziritaxestat in Patients with Idiopathic Pulmonary Fibrosis

Design, conduct, and interpretation of human mass balance studies and strategies for assessing metabolites-in-safety testing (MIST) in drug development

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