Celecoxib plus hormone therapy versus hormone therapy alone for hormone-sensitive prostate cancer: first results from the STAMPEDE multiarm, multistage, randomised controlled trial

Nicholas D James, Matthew R Sydes, Malcolm D Mason, Noel W Clarke, John Anderson, David P Dearnaley, John Dwyer, Gordana Jovic, Alastair W S Ritchie, J Martin Russell, Karen Sanders, George N Thalmann, Gianfilippo Bertelli, Alison J Birtle, Joe M O'Sullivan, Andrew Protheroe, Denise Sheehan, Narayanan Srihari, Mahesh K B Parmar, STAMPEDE investigators, Martin Russell, Malcolm Mason, Nicholas James, Noel Clarke, Andrew Protheroe, Denise Sheehan, David Dearnaley, Alison Birtle, Gianfilippo Bertelli, Joe O'Sullivan, Narayanan Srihari, Duncan McLaren, David Tsang, Anna Lydon, Catherine Ferguson, John Hetherington, Robert Laing, John Hardman, Simon Chowdhury, Stephanie Gibbs, Sharon Beesley, Santhanam Sundar, John Logue, Angus Robinson, Sue Brock, Prabir Chakraborti, Peter Hoskin, Isabel Syndikus, Prabir Chakraborti, Uschi Hofmann, Ashok Nikapota, John Graham, Omi Parikh, Ian Pedley, Noel Clarke, Helen Innes, Amit Bahl, Prakash Ramachandra, Robert Brierly, Audrey Cook, Catherine Heath, Andrew Protheroe, Neil McPhail, Fiona McKinna, Nishi Gupta, James Wylie, Joanna Gale, Paul Rogers, Jo Bowen, Rhona McMenemin, Priscilla Leone, William Cross, Stephen Harland, Sue Brock, Jawaher Ansari, David J Cole, Zafar Malik, Richard Shaffer, Jackie Newby, Asha Sivapalasuntharam, Hugh Newman, Robert Hughes, Michael Crawford, Natasha Mithal, Vijay Sangar, Sharon Beesley, Lisa Pickering, Maria Vilarino-Varela, John Hardman, Chester Countess, Azman Ibrahim, Andrew Protheroe, Tony Elliott, Royal Albert Edward Infirmary, Richard Cowan, Perric Crellin, Cathryn Woodward, William Harvey, Natasha Mithal, Simon Brown, Denise Sheehan, Alison Falconer, Daniel Saunders, Raeti Strebel, Daniel Engeler, George Thalmann, D Siciliano, Razvan Popescu, Nicholas D James, Matthew R Sydes, Malcolm D Mason, Noel W Clarke, John Anderson, David P Dearnaley, John Dwyer, Gordana Jovic, Alastair W S Ritchie, J Martin Russell, Karen Sanders, George N Thalmann, Gianfilippo Bertelli, Alison J Birtle, Joe M O'Sullivan, Andrew Protheroe, Denise Sheehan, Narayanan Srihari, Mahesh K B Parmar, STAMPEDE investigators, Martin Russell, Malcolm Mason, Nicholas James, Noel Clarke, Andrew Protheroe, Denise Sheehan, David Dearnaley, Alison Birtle, Gianfilippo Bertelli, Joe O'Sullivan, Narayanan Srihari, Duncan McLaren, David Tsang, Anna Lydon, Catherine Ferguson, John Hetherington, Robert Laing, John Hardman, Simon Chowdhury, Stephanie Gibbs, Sharon Beesley, Santhanam Sundar, John Logue, Angus Robinson, Sue Brock, Prabir Chakraborti, Peter Hoskin, Isabel Syndikus, Prabir Chakraborti, Uschi Hofmann, Ashok Nikapota, John Graham, Omi Parikh, Ian Pedley, Noel Clarke, Helen Innes, Amit Bahl, Prakash Ramachandra, Robert Brierly, Audrey Cook, Catherine Heath, Andrew Protheroe, Neil McPhail, Fiona McKinna, Nishi Gupta, James Wylie, Joanna Gale, Paul Rogers, Jo Bowen, Rhona McMenemin, Priscilla Leone, William Cross, Stephen Harland, Sue Brock, Jawaher Ansari, David J Cole, Zafar Malik, Richard Shaffer, Jackie Newby, Asha Sivapalasuntharam, Hugh Newman, Robert Hughes, Michael Crawford, Natasha Mithal, Vijay Sangar, Sharon Beesley, Lisa Pickering, Maria Vilarino-Varela, John Hardman, Chester Countess, Azman Ibrahim, Andrew Protheroe, Tony Elliott, Royal Albert Edward Infirmary, Richard Cowan, Perric Crellin, Cathryn Woodward, William Harvey, Natasha Mithal, Simon Brown, Denise Sheehan, Alison Falconer, Daniel Saunders, Raeti Strebel, Daniel Engeler, George Thalmann, D Siciliano, Razvan Popescu

Abstract

Background: Long-term hormone therapy alone is standard care for metastatic or high-risk, non-metastatic prostate cancer. STAMPEDE--an international, open-label, randomised controlled trial--uses a novel multiarm, multistage design to assess whether the early additional use of one or two drugs (docetaxel, zoledronic acid, celecoxib, zoledronic acid and docetaxel, or zoledronic acid and celecoxib) improves survival in men starting first-line, long-term hormone therapy. Here, we report the preplanned, second intermediate analysis comparing hormone therapy plus celecoxib (arm D) with hormone therapy alone (control arm A).

Methods: Eligible patients were men with newly diagnosed or rapidly relapsing prostate cancer who were starting long-term hormone therapy for the first time. Hormone therapy was given as standard care in all trial arms, with local radiotherapy encouraged for newly diagnosed patients without distant metastasis. Randomisation was done using minimisation with a random element across seven stratification factors. Patients randomly allocated to arm D received celecoxib 400 mg twice daily, given orally, until 1 year or disease progression (including prostate-specific antigen [PSA] failure). The intermediate outcome was failure-free survival (FFS) in three activity stages; the primary outcome was overall survival in a subsequent efficacy stage. Research arms were compared pairwise against the control arm on an intention-to-treat basis. Accrual of further patients was discontinued in any research arm showing safety concerns or insufficient evidence of activity (lack of benefit) compared with the control arm. The minimum targeted activity at the second intermediate activity stage was a hazard ratio (HR) of 0·92. This trial is registered with ClinicalTrials.gov, number NCT00268476, and with Current Controlled Trials, number ISRCTN78818544.

Findings: 2043 patients were enrolled in the trial from Oct 17, 2005, to Jan 31, 2011, of whom 584 were randomly allocated to receive hormone therapy alone (control group; arm A) and 291 to receive hormone therapy plus celecoxib (arm D). At the preplanned analysis of the second intermediate activity stage, with 305 FFS events (209 in arm A, 96 in arm D), there was no evidence of an advantage for hormone therapy plus celecoxib over hormone therapy alone: HR 0·94 (95% CI 0·74-1·20). [corrected]. 2-year FFS was 51% (95% CI 46-56) in arm A and 51% (95% CI 43-58) in arm D. There was no evidence of differences in the incidence of adverse events between groups (events of grade 3 or higher were noted at any time in 123 [23%, 95% CI 20-27] patients in arm A and 64 [25%, 19-30] in arm D). The most common grade 3-5 events adverse effects in both groups were endocrine disorders (55 [11%] of patients in arm A vs 19 [7%] in arm D) and musculoskeletal disorders (30 [6%] of patients in arm A vs 15 [6%] in arm D). The independent data monitoring committee recommended stopping accrual to both celecoxib-containing arms on grounds of lack of benefit and discontinuing celecoxib for patients currently on treatment, which was endorsed by the trial steering committee.

Interpretation: Celecoxib 400 mg twice daily for up to 1 year is insufficiently active in patients starting hormone therapy for high-risk prostate cancer, and we do not recommend its use in this setting. Accrual continues seamlessly to the other research arms and follow-up of all arms will continue to assess effects on overall survival.

Funding: Cancer Research UK, Pfizer, Novartis, Sanofi-Aventis, Medical Research Council (London, UK).

Copyright © 2012 Elsevier Ltd. All rights reserved.

Figures

Figure 1
Figure 1
Trial profile HT=hormone therapy. FFS=failure-free survival. *Two patients were excluded from the activity analysis in arm A because of errors in event dates that were unresolved at the time of this intermediate analysis. Both patients reported FFS events before randomisation. †Patients are conservatively excluded from the safety analysis if they have not returned follow-up data or reported a serious adverse event; this is expected since accrual was ongoing at the time of analysis and some patients would not have reached their first on-trial assessment point.
Figure 2
Figure 2
Time on celecoxib for patients in arm D (hormone therapy plus celecoxib) Only patients who reported starting celecoxib treatment are included. Patients still on celecoxib are censored at the date of last treatment. Patients were provided with sufficient tablets for 12 months of treatment. The drop at 12 months reflects patients completing their trial treatment; events before then represent patients stopping trial treatment sooner, for any reason.
Figure 3
Figure 3
Kaplan-Meier curve of failure-free survival in arm A (hormone therapy alone) versus arm D (hormone therapy plus celecoxib) HT=hormone therapy. C=celecoxib.

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