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Cabazitaxel Versus Abiraterone or Enzalutamide for Poor-prognosis Metastatic Castration-resistant Prostate Cancer After Docetaxel: A Phase 2 Trial with a Circulating Tumor DNA Analysis.

Karan Parekh ,
Kim van der Zande ,
Sarah W S Ng ,
Cameron Herberts ,
Edmond M Kwan ,
Gillian Vandekerkhove ,
Vincent van der Noort ,
Milou P H Busard ,
Aart Beeker ,
Pieter van den Berg ,
Jeantine M de Feijter ,
Vincent Dezentje ,
Paul Hamberg ,
Danny Houtsma ,
Suzan Ras ,
Metin Tascilar ,
Rebecca D Tutuhatunewa-Louhanepessy ,
Yi Jou Ruby Liao ,
Sofie H Tolmeijer ,
Gráinne Donnellan ,
Kim N Chi ,
Alexander W Wyatt ,
Wilbert Zwart ,
Andries M Bergman ,

Abstract

METHODS

A multicenter, open-label, phase 2b trial randomized poor-prognosis mCRPC patients to an ARPI (1000 mg abiraterone plus prednisone or 160 mg enzalutamide daily) or cabazitaxel (25 mg/m2 every 3 wk plus prednisone daily). The primary endpoint was the clinical benefit rate (CBR) at 12 wk. The secondary endpoints included radiographic progression-free survival (rPFS), overall survival (OS), and PSA50 response. Genomic analyses on plasma utilized targeted cell-free DNA sequencing at baseline, 12 wk, and progression.

CONCLUSIONS AND CLINICAL IMPLICATIONS

No significant differences in CBR or time-to-event endpoints were observed between cabazitaxel and ARPIs. However, prior ARPI exposure, a higher baseline ctDNA fraction, and PTEN alterations were strongly prognostic.

BACKGROUND AND OBJECTIVE

Whether cabazitaxel or an androgen receptor pathway inhibitor (ARPI) is the optimal treatment option for poor-prognosis metastatic castration-resistant prostate cancer (mCRPC), progressing on docetaxel, remains unclear. There are limited prospective data supporting a preference for one of these treatments and few candidate biomarkers to inform individual patient management. This study aims to compare the clinical efficacy of cabazitaxel versus ARPIs in patients with poor-prognosis mCRPC who have progressed on docetaxel, and to evaluate the prognostic and predictive utility of circulating tumor DNA (ctDNA) in this treatment-refractory population.

KEY FINDINGS AND LIMITATIONS

In total, 106 patients were randomized. The CBR at 12 wk was 62.3% (66/106), with no difference between treatments (p = 0.54). Between groups, rPFS and OS (median follow-up of 30.9 mo) were not different. PSA50 was higher in the ARPI arm (47.2%) than in the cabazitaxel arm (26.9%; p = 0.04). Prior ARPI exposure (in 37.7%) predicted inferior outcomes on ARPIs but not on cabazitaxel. Adverse events of grade ≥3 were more frequent with cabazitaxel (65.4% vs 30.2%). A high baseline ctDNA fraction correlated with reduced rPFS and OS; plasma AR copy number status was not associated with outcomes, but PTEN alterations were linked with shorter OS (hazard ratio: 1.9, multivariable p = 0.02).

More about this publication

European urology oncology

Volume 9
Issue nr. 2
Pages 328-345
Publication date 01-04-2026

Full text links

Publisher website (DOI) 10.1016/j.euo.2025.07.006
Europe PubMed Central 41033927
Pubmed 41033927

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