Phase II pilot study of the prednisone to dexamethasone switch in metastatic castration-resistant prostate cancer (mCRPC) patients with limited progression on abiraterone plus prednisone (SWITCH study)

Nuria Romero-Laorden,Fernando López-Campos,Pedro P López,Ylenia Cendón,Juan-Jesús Cruz,Teresa Garcés,Ma Paz Nombela,Bernardo Herrera,Gerhardt Attard,Floortje Van De Poll,Adriana Rosero,David Lorente,Anuradha Jayaram,María Isabel Corbí Sáez ,G Grau ,L Rivera ,A Montesa ,R Villatoro ,R Correa ,M.i Pacheco ,Rebeca Lozano,Ana Gutierrez-Pecharoman,Elena Castro,David Olmos

doi:10.1038/s41416-018-0123-9

Abstract

BackgroundDespite most metastatic castration-resistant prostate cancer (mCRPC) patients benefit from abiraterone acetate plus prednisone 5 mg bid (AA + P), resistance eventually occurs. Long-term use of prednisone has been suggested as one of the mechanisms driving resistance, which may be reversed by switching to another steroid.MethodsSWITCH was a single-arm, open-label, single-stage phase II study. The primary objective was to evaluate the antitumour activity of abiraterone acetate plus dexamethasone 0.5 mg daily (AA + D) in mCRPC patients progressing to AA + P. Clinically stable mCRPC patients who had prostate-specific antigen (PSA) and/or limited radiographic progression after at least 12 weeks on AA + P, were eligible. The primary endpoint was measured as the proportion of patients achieving a PSA decline of ≥ 30% (PSA30) from baseline after 6 weeks on AA + D. Secondary endpoints included: PSA50 response rate at 12 weeks, time to biochemical and radiological progression, overall survival, safety profile evaluation, benefit from subsequent treatment lines and the identification of biomarkers of response (AR copy number, TMPRSS2-ERG status and PTEN expression).ResultsTwenty-six patients were enrolled. PSA30 and PSA50 were 46.2% and 34.6%, respectively. Median time to biochemical and radiological progression were 5.3 and 11.8 months, respectively. Two radiological responses were observed. Median overall survival was 20.9 months. Patients with AR gain detected in plasma circulating tumour DNA did not respond to switch, whereas patients with AR normal status benefited the most. No significant toxicities were observed and PSA50 response rate to subsequent taxane was 50%.ConclusionsIn selected clinical stable mCRPC patients with limited disease progression on AA + P, a steroid switch from prednisone to dexamethasone can lead to PSA and radiological responses.

Highlights

INTRODUCTION novel therapeutic options are being developed for metastatic castration-resistant prostate cancer, new rational-based strategies may optimise the benefit from currently available therapies such as abiraterone acetate (AA)[1,2]
Castrate metastatic prostate cancer patients with Eastern Cooperative Oncology Group (ECOG) performance status 0–2 who had a histological diagnosis of prostate adenocarcinoma, a prostate-specific antigen (PSA) > 2 ng/mL, and confirmed biochemical progression as defined by PCWG2 criteria[10] after at least 12 weeks of AA 1000 mg od and prednisone 5 mg bid were eligible
Patient characteristics Twenty-six metastatic castration-resistant prostate cancer (mCRPC) patients were enrolled in this Phase II trial between June 2013 and March 2016 (CONSORT diagram supplementary appendix S3)

Summary

Introduction

Novel therapeutic options are being developed for metastatic castration-resistant prostate cancer (mCRPC), new rational-based strategies may optimise the benefit from currently available therapies such as abiraterone acetate (AA)[1,2].AA inhibits androgen synthesis through blockade of CYP17 17αhidroxylase and 17,20-lyase functions. Despite most metastatic castration-resistant prostate cancer (mCRPC) patients benefit from abiraterone acetate plus prednisone 5 mg bid (AA + P), resistance eventually occurs. The primary objective was to evaluate the antitumour activity of abiraterone acetate plus dexamethasone 0.5 mg daily (AA + D) in mCRPC patients progressing to AA + P. Stable mCRPC patients who had prostate-specific antigen (PSA) and/or limited radiographic progression after at least 12 weeks on AA + P, were eligible. Secondary endpoints included: PSA50 response rate at 12 weeks, time to biochemical and radiological progression, overall survival, safety profile evaluation, benefit from subsequent treatment lines and the identification of biomarkers of response (AR copy number, TMPRSS2-ERG status and PTEN expression). CONCLUSIONS: In selected clinical stable mCRPC patients with limited disease progression on AA + P, a steroid switch from prednisone to dexamethasone can lead to PSA and radiological responses

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