Effects of the endpoint adjudication process on the results of a randomised controlled trial: The ADVANCE trial

Andre Pascal Kengne; Anushka Patel; Bruce Neal; Carol Pollock; CB Granger; Craig Anderson; Giuseppe Mancia; Greg Fulcher; Hisatomi Arima; Isabelle Boutron; J Pogue; JG Cleland; JL Petersen; John Chalmers; John Watson; Jun Hata; KW Mahaffey; KW Mahaffey; KW Mahaffey; Mark Adams; Mark Woodward; Neil Poulter; Rohina Joshi; SD Walter; Sophia Zoungas; Stephen MacMahon; T Ninomiya; Toshiharu Ninomiya; U Näslund

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Effects of the endpoint adjudication process on the results of a randomised controlled trial: The ADVANCE trial

Authors: Andre Pascal Kengne
Anushka Patel
Bruce Neal
Carol Pollock
CB Granger
Craig Anderson
Giuseppe Mancia
Greg Fulcher
Hisatomi Arima
Isabelle Boutron
J Pogue
JG Cleland
JL Petersen
John Chalmers
John Watson
Jun Hata
KW Mahaffey
KW Mahaffey
KW Mahaffey
Mark Adams
Mark Woodward
Neil Poulter
Rohina Joshi
SD Walter
Sophia Zoungas
Stephen MacMahon
T Ninomiya
Toshiharu Ninomiya
U Näslund
Publication date: 1 January 2013
Publisher: 'Public Library of Science (PLoS)'
Doi

Abstract

BACKGROUND Endpoint adjudication committees (EPAC) are widely used in clinical trials. The aim of the present analysis is to assess the effects of the endpoint adjudication process on the main findings of the ADVANCE trial (Trial registration: ClinicalTrials.gov NCT00145925). METHODS AND FINDINGS The ADVANCE trial was a multicentre, 2×2 factorial randomised controlled trial of blood pressure lowering and intensive blood glucose control in 11140 patients with type 2 diabetes. Primary outcomes were major macrovascular (nonfatal myocardial infarction, nonfatal stroke and cardiovascular death) and microvascular (new or worsening nephropathy and retinopathy) events. Suspected primary outcomes were initially reported by the investigators at the 215 sites with subsequent adjudication by the EPAC. The EPAC also adjudicated upon potential events identified directly by ongoing screening of all reported events. Over a median follow-up of 5 years, the site investigators reported one or more primary outcomes among 2443 participants. After adjudication these events were confirmed for 2077 (85%) with 48 further events added through the EPAC-led database screening process. The estimated relative risk reductions (95% confidence intervals) in the primary outcome for the blood pressure lowering comparison were 8% (−1 to 15%) based on the investigator-reported events and 9% (0 to 17%) based on the EPAC-based events (P for homogeneity = 0.70). The corresponding findings for the glucose comparison were 8% (1 to 15%) and 10% (2% to 18%) (P for homogeneity = 0.60). The effect estimates were also highly comparable when studied separately for macrovascular events and microvascular events for both comparisons (all P for homogeneity>0.6). CONCLUSIONS The endpoint adjudication process had no discernible impact on the main findings in ADVANCE. These data highlight the need for careful consideration of the likely impact of an EPAC on the findings and conclusions of clinical trials prior to their establishment.Jun Hata, Hisatomi Arima, Sophia Zoungas,, Greg Fulcher, Carol Pollock, Mark Adams, John Watson, Rohina Joshi, Andre Pascal Kengne, Toshiharu Ninomiya, Craig Anderson, Mark Woodward, Anushka Patel, Giuseppe Mancia, Neil Poulter, Stephen MacMahon, John Chalmers, Bruce Neal, on behalf of the ADVANCE Collaborative Grou