Evaluation of 1β-Hydroxylation of Deoxycholic Acid as a Non-Invasive Urinary Biomarker of CYP3A Activity in the Assessment of Inhibition-Based Drug–Drug Interaction in Healthy Volunteers

• Published in: Journal of personalized medicine Vol. 11; no. 6; p. 457
• Main Authors: Li, Xue-Qing, Thelingwani, Roslyn Stella, Bertilsson, Leif, Diczfalusy, Ulf, Andersson, Tommy B., Masimirembwa, Collen
• Format: Journal Article
• Language: English
• Published: Basel MDPI AG 24.05.2021; MDPI
• Subjects: Acids; Alprazolam; Biomarkers; Consent; Cytochrome P450; Deoxycholic acid; Drug interaction; Drug interactions; Enzymes; Exploratory behavior; Fluconazole; Hepatitis; Hormones; Hydroxylation; Itraconazole; Laboratories; Medical research; Medicin och hälsovetenskap; Metabolism; Metabolites; Midazolam; Pharmaceuticals; Plasma; Precision medicine; Sample size; Urine; Values; Canada; Zimbabwe; United Kingdom > UK; United States > US
• ISSN: 2075-4426; 2075-4426
• DOI: 10.3390/jpm11060457

In this study, we aimed to evaluate the utility of endogenous 1β-hydroxy-deoxycholic acid/total deoxycholic acid ratio (1β-OH-DCA/ToDCA) in spot urine as a surrogate marker of cytochrome P450 3A (CYP3A) activity in the assessment inhibition-based drug–drug interactions in healthy volunteers. This was accomplished through an open-label, three-treatment parallel-arm study in healthy male volunteers from Zimbabwe. Each group received itraconazole (ITZ; 100 mg once daily; n = 10), fluconazole (FKZ; 50 mg once daily; n = 9), or alprazolam (APZ; 1 mg once daily; n = 8) orally. Midazolam (MDZ), dosed orally and intravenously, was used as a comparator to validate the exploratory measures of CYP3A activity and the effects of known inhibitors. Urinary metabolic ratios of 1β-OH-DCA/ToDCA before and after CYP3A inhibitor treatment showed a similar magnitude of inhibitory effects of the three treatments as that measured by oral MDZ clearance. The maximum inhibition effect of a 75% reduction in the 1β-OH-DCA/ToDCA ratio compared to the baseline was achieved in the ITZ group following six once-daily doses of 100 mg. The correlations of the two markers for CYP3A inhibitor treatment were significant (rs = 0.53, p < 0.01). The half-life of urinary endogenous 1β-OH-DCA/ToDCA was estimated as four days. These results suggested that 1β-OH-DCA/ToDCA in spot urine is a promising convenient, non-invasive, sensitive, and relatively quickly responsive endogenous biomarker that can be used for CYP3A inhibition-based drug–drug interaction in clinical studies.