Abstract
INTRODUCTION: WK0202, a β-lapachone derivative under clinical development, activates NAD(P)H quinone dehydrogenase 1 (NQO1), acting as a detoxifying and antioxidant agent. In this study, a metabolomics investigation of β-lapachone derivatives in humans is performed to characterize drug-induced alterations in endogenous metabolic pathways. OBJECTIVES: This study investigated metabolic alterations induced by WK0202 administration and their potential association with its therapeutic mechanism and efficacy. Using targeted and untargeted metabolomics approaches, we identified potential pharmacodynamic biomarker candidates that may reflect the drug's activity and metabolic effects. METHODS: Plasma samples from healthy subjects who received multiple doses of WK0202 were compared with a placebo control group. The metabolomic profiles were compared pre- and post-dose to identify significant metabolic changes. Significant metabolites were identified using statistical analyses, focusing on key metabolic pathways. To further investigate NQO1 genotype effects, Spearman correlation analysis was performed between post/pre-dose concentration ratios and genotypes. RESULTS: Following WK0202 administration, significant changes were observed in the alanine, aspartate and glutamate metabolism, arginine biosynthesis, and lipid metabolism. Although most metabolites were not strongly dependent on NQO1 genotype or dose group, they exhibited an overall consistent trend. These alterations were indicative of Nrf2 pathway activation, possibly by NQO1-mediated drug activity. CONCLUSION: These metabolic alterations highlight the potential of endogenous metabolites as surrogate markers for identifying novel therapeutic targets and assessing the efficacy of WK0202 in future clinical studies.