Addition of docetaxel to hormonal therapy in low- and high-burden metastatic hormone sensitive prostate cancer: long-term survival results from the STAMPEDE trial

Noel W. Clarke,Adnan Ali,F C Ingleby,Alex P. Hoyle,Claire Amos,Gerhardt Attard,Christopher D Brawley,J Calvert,S. Chowdhury,Adrian Cook,W Cross,David P. Dearnaley,H Douis,Duncan C. Gilbert,Silke Gillessen,Robert Jones,R.E. Langley,Archie Macnair,Zafar Malik,Malcolm David Mason,David Matheson,Robin Millman,Chris Parker,A. W. S. Ritchie,Hannah L. Rush,J.M. Russell,Janet E. Brown,S. Beesley,Alison J. Birtle,L. Capaldi,Joanna Gale,S. Gibbs,Anna Lydon,A. Nikapota,Aurelius Omlin,Joe M. O’Sullivan,Omi Parikh,Andrew Protheroe,Sarah Rudman,Narayanan Srihari,Matthew S. Simms,J. S. Tanguay,S. Tolan,John Wagstaff,Jan Wallace,James D. Wylie,Anjali Zarkar,Matthew R. Sydes,M.K.B. Parmar,Nicholas D. James

Addition of docetaxel to hormonal therapy in low- and high-burden metastatic hormone sensitive prostate cancer: long-term survival results from the STAMPEDE trial

2019

Abstract Background STAMPEDE has previously reported that the use of upfront docetaxel improved overall survival (OS) for metastatic hormone naive prostate cancer patients starting long-term androgen deprivation therapy. We report on long-term outcomes stratified by metastatic burden for M1 patients. Methods We randomly allocated patients in 2 : 1 ratio to standard-of-care (SOC; control group) or SOC + docetaxel. Metastatic disease burden was categorised using retrospectively-collected baseline staging scans where available. Analysis used Cox regression models, adjusted for stratification factors, with emphasis on restricted mean survival time where hazards were non-proportional. Results Between 05 October 2005 and 31 March 2013, 1086 M1 patients were randomised to receive SOC (n = 724) or SOC + docetaxel (n = 362). Metastatic burden was assessable for 830/1086 (76%) patients; 362 (44%) had low and 468 (56%) high metastatic burden. Median follow-up was 78.2 months. There were 494 deaths on SOC (41% more than the previous report). There was good evidence of benefit of docetaxel over SOC on OS (HR = 0.81, 95% CI 0.69–0.95, P = 0.009) with no evidence of heterogeneity of docetaxel effect between metastatic burden sub-groups (interaction P = 0.827). Analysis of other outcomes found evidence of benefit for docetaxel over SOC in failure-free survival (HR = 0.66, 95% CI 0.57–0.76, P 0.5 in each case). There was no evidence that docetaxel resulted in late toxicity compared with SOC: after 1 year, G3-5 toxicity was reported for 28% SOC and 27% docetaxel (in patients still on follow-up at 1 year without prior progression). Conclusions The clinically significant benefit in survival for upfront docetaxel persists at longer follow-up, with no evidence that benefit differed by metastatic burden. We advocate that upfront docetaxel is considered for metastatic hormone naive prostate cancer patients regardless of metastatic burden.

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