Pharmacometabolomics of trabectedin in metastatic soft tissue sarcoma patients

Giuseppe Corona; Emanuela Di Gregorio; Angela Buonadonna; Davide Lombardi; Simona Scalone; Agostino Steffan; Gianmaria Miolo

doi:10.3389/fphar.2023.1212634

Pharmacometabolomics of trabectedin in metastatic soft tissue sarcoma patients

Front Pharmacol. 2023 Aug 11:14:1212634. doi: 10.3389/fphar.2023.1212634. eCollection 2023.

Authors

Giuseppe Corona¹, Emanuela Di Gregorio¹, Angela Buonadonna², Davide Lombardi², Simona Scalone², Agostino Steffan¹, Gianmaria Miolo²

Affiliations

¹ Immunopathology and Cancer Biomarkers Unit, Centro di Riferimento Oncologico di Aviano (CRO), IRCCS, Aviano, Italy.
² Medical Oncology and Cancer Prevention Unit, Centro di Riferimento Oncologico di Aviano (CRO), IRCCS, Aviano, Italy.

Abstract

Objective: Trabectedin is an anti-cancer drug commonly used for the treatment of patients with metastatic soft tissue sarcoma (mSTS). Despite its recognized efficacy, significant variability in pharmacological response has been observed among mSTS patients. To address this issue, this pharmacometabolomics study aimed to identify pre-dose plasma metabolomics signatures that can explain individual variations in trabectedin pharmacokinetics and overall clinical response to treatment. Methods: In this study, 40 mSTS patients treated with trabectedin administered by 24 h-intravenous infusion at a dose of 1.5 mg/m² were enrolled. The patients' baseline plasma metabolomics profiles, which included derivatives of amino acids and bile acids, were analyzed using multiple reaction monitoring LC-MS/MS together with their pharmacokinetics profile of trabectedin. Multivariate Partial least squares regression and univariate statistical analyses were utilized to identify correlations between baseline metabolite concentrations and trabectedin pharmacokinetics, while Partial Least Squares-Discriminant Analysis was employed to evaluate associations with clinical response. Results: The multiple regression model, derived from the correlation between the AUC of trabectedin and pre-dose metabolomics, exhibited the best performance by incorporating cystathionine, hemoglobin, taurocholic acid, citrulline, and the phenylalanine/tyrosine ratio. This model demonstrated a bias of 4.6% and a precision of 17.4% in predicting drug AUC, effectively accounting for up to 70% of the inter-individual pharmacokinetic variability. Through the use of Partial least squares-Discriminant Analysis, cystathionine and hemoglobin were identified as specific metabolic signatures that effectively distinguish patients with stable disease from those with progressive disease. Conclusions: The findings from this study provide compelling evidence to support the utilization of pre-dose metabolomics in uncovering the underlying causes of pharmacokinetic variability of trabectedin, as well as facilitating the identification of patients who are most likely to benefit from this treatment.

Keywords: biomarkers; metabolomics; pharmacodynamics; pharmacokinetics; pharmacometabolomics; sarcoma; trabectedin.

Grants and funding

The study was supported by the Italian Ministry of Health-Ricerca Corrente.