Aspirin as an adjuvant treatment for cancer : feasibility results from the Add-Aspirin randomised trial
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Joharatnam-Hogan, NalinieCafferty, Fay
Hubner, Richard
Swinson, Daniel
Sothi, Sharmila
Gupta, Kamalnayan
Falk, Stephen
Patel, Kinnari
Warner, Nicola
Kunene, Victoria
Rowley, Sam
Khabra, Komel
Underwood, Tim
Jankowski, Janusz
Bridgewater, John
Crossley, Anne
Henson, Verity
Berkman, Lindy
Gilbert, Duncan
Kynaston, Howard
Ring, Alistair
Cameron, David
Din, Farhat
Graham, Janet
Iveson, Timothy
Adams, Richard
Thomas, Anne
Wilson, Richard
Pramesh, C S
Langley, Ruth
Affiliation
University College London; The Christie Hospital; St James University Hospital; University Hospital Coventry and Warwickshire; Worcestershire Royal Hospital; Bristol Haematology & Oncology Centre; Churchill Hospital; Stoke Mandeville Hospital; Walsall Healthcare NHS Trust; University of Southampton; Morecambe Bay University Hospitals NHS Trust; National Institute for Health and Care Excellence; NCRI Consumer Liaison Group; Cardiff University; Royal Marsden Hospital; Cancer Research UK Edinburgh Centre; Western General Hospital; Beatson West of Scotland Cancer Centre; Southampton General Hospital; Velindre Cancer Centre; Leicester Royal Infirmary; University of Glasgow; Tata Memorial HospitalPublication date
2019-08-30
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Background: Preclinical, epidemiological, and randomised data indicate that aspirin might prevent tumour development and metastasis, leading to reduced cancer mortality, particularly for gastro-oesophageal and colorectal cancer. Randomised trials evaluating aspirin use after primary radical therapy are ongoing. We present the pre-planned feasibility analysis of the run-in phase of the Add-Aspirin trial to address concerns about toxicity, particularly bleeding after radical treatment for gastro-oesophageal cancer. Methods: The Add-Aspirin protocol includes four phase 3 randomised controlled trials evaluating the effect of daily aspirin on recurrence and survival after radical cancer therapy in four tumour cohorts: gastro-oesophageal, colorectal, breast, and prostate cancer. An open-label run-in phase (aspirin 100 mg daily for 8 weeks) precedes double-blind randomisation (for participants aged under 75 years, aspirin 300 mg, aspirin 100 mg, or matched placebo in a 1:1:1 ratio; for patients aged 75 years or older, aspirin 100 mg or matched placebo in a 2:1 ratio). A preplanned analysis of feasibility, including recruitment rate, adherence, and toxicity was performed. The trial is registered with the International Standard Randomised Controlled Trials Number registry (ISRCTN74358648) and remains open to recruitment. Findings: After 2 years of recruitment (October, 2015, to October, 2017), 3494 participants were registered (115 in the gastro-oesophageal cancer cohort, 950 in the colorectal cancer cohort, 1675 in the breast cancer cohort, and 754 in the prostate cancer cohort); 2719 (85%) of 3194 participants who had finished the run-in period proceeded to randomisation, with rates consistent across tumour cohorts. End of run-in data were available for 2253 patients; 2148 (95%) of the participants took six or seven tablets per week. 11 (0·5%) of the 2253 participants reported grade 3 toxicity during the run-in period, with no upper gastrointestinal bleeding (any grade) in the gastro-oesophageal cancer cohort. The most frequent grade 1-2 toxicity overall was dyspepsia (246 [11%] of 2253 participants). Interpretation: Aspirin is well-tolerated after radical cancer therapy. Toxicity has been low and there is no evidence of a difference in adherence, acceptance of randomisation, or toxicity between the different cancer cohorts. Trial recruitment continues to determine whether aspirin could offer a potential low cost and well tolerated therapy to improve cancer outcomes.Citation
Joharatnam-Hogan N, Cafferty F, Hubner R, Swinson D, Sothi S, Gupta K, Falk S, Patel K, Warner N, Kunene V, Rowley S, Khabra K, Underwood T, Jankowski J, Bridgewater J, Crossley A, Henson V, Berkman L, Gilbert D, Kynaston H, Ring A, Cameron D, Din F, Graham J, Iveson T, Adams R, Thomas A, Wilson R, Pramesh CS, Langley R; Add-Aspirin Trial Management Group. Aspirin as an adjuvant treatment for cancer: feasibility results from the Add-Aspirin randomised trial. Lancet Gastroenterol Hepatol. 2019 Nov;4(11):854-862.Type
ArticlePMID
31477558Publisher
Elsevierae974a485f413a2113503eed53cd6c53
10.1016/S2468-1253(19)30289-4