TY - JOUR
T1 - Reporting of surrogate endpoints in randomised controlled trial protocols (SPIRIT-Surrogate): extension checklist with explanation and elaboration
AU - Manyara, Anthony Muchai
AU - Davies, Philippa
AU - Stewart, Derek
AU - Weir, Christopher J
AU - Young, Amber E
AU - Blazeby, Jane
AU - Butcher, Nancy J
AU - Bujkiewicz, Sylwia
AU - Chan, An-Wen
AU - Dawoud, Dalia
AU - Offringa, Martin
AU - Ouwens, Mario
AU - Hróbjartssson, Asbjørn
AU - Amstutz, Alain
AU - Bertolaccini, Luca
AU - Bruno, Vito Domenico
AU - Devane, Declan
AU - Faria, Christina D C M
AU - Gilbert, Peter B
AU - Harris, Ray
AU - Lassere, Marissa
AU - Marinelli, Lucio
AU - Markham, Sarah
AU - Powers, John H
AU - Rezaei, Yousef
AU - Richert, Laura
AU - Schwendicke, Falk
AU - Tereshchenko, Larisa G
AU - Thoma, Achilles
AU - Turan, Alparslan
AU - Worrall, Andrew
AU - Christensen, Robin
AU - Collins, Gary S
AU - Ross, Joseph S
AU - Taylor, Rod S
AU - Oriana, Ciani
N1 - Publisher Copyright:
© 2019 Author(s).
PY - 2024/7/9
Y1 - 2024/7/9
N2 - Randomised controlled trials often use surrogate endpoints to substitute for a target outcome (an outcome of direct interest and relevance to trial participants, clinicians, and other stakeholders—eg, all cause mortality) to improve efficiency (through shortened duration of follow-up, reduced sample size, and lower research costs), and for ethical or practical reasons. However, their use has a fundamental limitation in terms of uncertainty of the intervention effect on the target outcome and limited information on potential intervention harms. There have been increasing calls for improved reporting of trial protocols that use surrogate endpoints. This report presents the SPIRIT-Surrogate, an extension of the Standard Protocol Items: Recommendations for Interventional Trials (SPIRIT) checklist, a consensus driven reporting guideline designed for trial protocols using surrogate endpoints as the primary outcome(s). The SPIRIT-Surrogate extension includes nine items modified from the SPIRIT 2013 checklist. The guideline provides examples and explanations for each item. We recommend that all stakeholders (including trial investigators and sponsors, research ethics reviewers, funders, journal editors, and peer reviewers) use this extension in reporting trial protocols that use surrogate endpoints. Its use will allow for improved design of such trials, improved transparency, and interpretation of findings when trials are completed, and ultimately reduced research waste.
AB - Randomised controlled trials often use surrogate endpoints to substitute for a target outcome (an outcome of direct interest and relevance to trial participants, clinicians, and other stakeholders—eg, all cause mortality) to improve efficiency (through shortened duration of follow-up, reduced sample size, and lower research costs), and for ethical or practical reasons. However, their use has a fundamental limitation in terms of uncertainty of the intervention effect on the target outcome and limited information on potential intervention harms. There have been increasing calls for improved reporting of trial protocols that use surrogate endpoints. This report presents the SPIRIT-Surrogate, an extension of the Standard Protocol Items: Recommendations for Interventional Trials (SPIRIT) checklist, a consensus driven reporting guideline designed for trial protocols using surrogate endpoints as the primary outcome(s). The SPIRIT-Surrogate extension includes nine items modified from the SPIRIT 2013 checklist. The guideline provides examples and explanations for each item. We recommend that all stakeholders (including trial investigators and sponsors, research ethics reviewers, funders, journal editors, and peer reviewers) use this extension in reporting trial protocols that use surrogate endpoints. Its use will allow for improved design of such trials, improved transparency, and interpretation of findings when trials are completed, and ultimately reduced research waste.
U2 - 10.1136/bmj-2023-078525
DO - 10.1136/bmj-2023-078525
M3 - Article (Academic Journal)
C2 - 38981624
SN - 0959-8138
VL - 386
JO - BMJ
JF - BMJ
M1 - e078525
ER -