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Reporting of randomised trials

Published online by Cambridge University Press:  02 January 2018

A. K. Jainer  and
S. Acharya
A. K. Jainer
Affiliation:
St Michael's Hospital, St Michael's Road, South Warwick Combined Trust, South Warwick CV34 5QW, UK
S. Acharya
Affiliation:
St Michael's Hospital, St Michael's Road, South Warwick Combined Trust, South Warwick CV34 5QW, UK
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Abstract

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The British Journal of Psychiatry , Volume 180 , Issue 2 , February 2002 , pp. 185
Copyright
Copyright © Royal College of Psychiatrists, 2002 

Allgulander et al (Reference Allgulander, Hackett and Salinas2001) evaluated the efficacy of venlafaxine extended release (ER) in patients with generalised anxiety disorder and reported that all doses of venlafaxine ER showed significantly higher treatment response rates compared with placebo. We read this double-blind, randomised study with great interest and wish to raise concerns about the recruitment of the subjects. Randomised controlled trials are always cited as the gold standard for detecting the efficacy of results. However, they often can be flawed in design and are not immune to bias. Large-scale multi-centre trials often include hundreds of patients from a large number of centres located in different countries. The clinical relevance of such studies has been criticised on the grounds of selection bias.

Healy (Reference Healy2001) stated that company-sponsored randomised controlled trials invariably recruit samples of convenience, which by definition do not really sustain extrapolation to normal clinical practice. These trials also make use of restrictive inclusion criteria in order to ensure the greatest possible homogeneity of the sample studied. This creates a problem when attempting to generalise the results from available trials to more everyday patient populations.

In this context, the Consolidated Standards of Reporting Trials (CONSORT) guidelines, which state that all patients assessed for the trial should be accounted for and that the report should be accompanied by a diagram which explains what happened to all the patients involved in the trial (Reference Begg, Cho and EastwoodBegg et al, 1996), should be followed. Allgulander et al failed to follow the CONSORT guidelines. The information about recruitment of the subjects is lacking. We do not know how many subjects were initially assessed, how many were excluded and why. We also do not have any idea of the response rate or the participation rate, which have implications for generalisability and future research. Also, patients with significant depressive symptomatology were excluded, which raises concerns over whether these results are relevant to general patients.

Footnotes

EDITED BY MATTHEW HOTOPF

References

Allgulander, C., Hackett, D. & Salinas, E. (2001) Venlafaxine extended release (ER) in the treatment of generalised anxiety disorder. Twenty-four-week placebo-controlled dose-ranging study. British Journal of Psychiatry, 179, 1522.CrossRefGoogle Scholar
Begg, C., Cho, M. & Eastwood, S. (1996) Improving the quality of reporting of randomized controlled trials: the CONSORT statement. JAMA, 276, 637639.CrossRefGoogle ScholarPubMed
Healy, D. (2001) Evidence biased psychiatry? Psychiatric Bulletin, 265, 290291.CrossRefGoogle Scholar
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