How do researchers determine the difference to be detected in superiority trials? Results of a survey from a panel of researchers

Angèle Gayet-Ageron; Anne-Sophie Jannot; Thomas Agoritsas; Sandrine Rudaz; Christophe Combescure; Thomas Perneger

doi:10.1186/s12874-016-0195-2

BMC Medical Research Methodology (Jul 2016)

How do researchers determine the difference to be detected in superiority trials? Results of a survey from a panel of researchers

Angèle Gayet-Ageron,
Anne-Sophie Jannot,
Thomas Agoritsas,
Sandrine Rudaz,
Christophe Combescure,
Thomas Perneger

Affiliations

Angèle Gayet-Ageron: Division of clinical-epidemiology, Department of health and community medicine, University of Geneva & University Hospitals of Geneva
Anne-Sophie Jannot: Department of Medical Informatics and Public Health, Hôpital Européen Georges Pompidou, Assistance Publique Hôpitaux de Paris
Thomas Agoritsas: Division of clinical-epidemiology, Department of health and community medicine, University of Geneva & University Hospitals of Geneva
Sandrine Rudaz: Division of clinical-epidemiology, Department of health and community medicine, University of Geneva & University Hospitals of Geneva
Christophe Combescure: Division of clinical-epidemiology, Department of health and community medicine, University of Geneva & University Hospitals of Geneva
Thomas Perneger: Division of clinical-epidemiology, Department of health and community medicine, University of Geneva & University Hospitals of Geneva

DOI: https://doi.org/10.1186/s12874-016-0195-2
Journal volume & issue: Vol. 16, no. 1
pp. 1 – 10

Abstract

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Abstract Background There is currently no guidance for selecting a specific difference to be detected in a superiority trial. We explored 3 factors that in our opinion should influence the difference to be detected (type of outcome, patient age group, and presence of treatment side-effects), and 3 that should not (baseline level of risk, logistical difficulties, and cost of treatment). Methods We conducted an experimental survey using a factorial design among 380 corresponding authors of randomized controlled trials indexed in Medline. Two hypothetical vignettes were submitted to participants: one described a trial of a new analgesic in mild trauma injuries, the other described a trial of a new chemotherapy among cancer patients. The first vignette tested the baseline level of risk, patient age-group, patient recruitment difficulties, and treatment side-effects. The second tested the baseline level of risk, patient age-group, type of outcome, and cost of treatment. The respondents were asked to select the smallest gain of effectiveness that should be detected by the trial. Results In vignette 1, respondents selected a median difference to be detected corresponding to an improvement of 7.0 % in pain control with the new treatment. In vignette 2, they selected a median difference to be detected corresponding to a reduction of 5.0 % in mortality or cancer recurrence with the new chemotherapy. In both vignettes, the difference to be detected decreased significantly with the baseline risk. The other factor influencing difference to be detected was the age group, but the impact of this factor was smaller. Cost, side-effects, outcome severity, or mention of logistical difficulties did not significantly impact the difference to be detected selected by participants. Conclusions Three of the anticipated effects conformed to our expectations (the effect of patient age, and absence of effect of the cost of treatment and of patient recruitment difficulties) and the other three did not. These findings can guide future research in determining differences to be detected in trials that can translate to meaningful clinical decision-making.

Published in BMC Medical Research Methodology

ISSN: 1471-2288 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General)
Website: http://bmcmedresmethodol.biomedcentral.com

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