Systematic Review and Meta-Analysis of Randomised, Other-than-Placebo Controlled, Trials of Individualised Homeopathic Treatment

Robert T. Mathie; Susanne Ulbrich-Zürni; Petter Viksveen; E. Rachel Roberts; Elizabeth S. Baitson; Lynn A. Legg; Jonathan R. T. Davidson

doi:10.1055/s-0038-1667129

Homeopathy, Table of Contents

Homeopathy 2018; 107(04): 229-243
DOI: 10.1055/s-0038-1667129

Review Article

The Faculty of Homeopathy

Systematic Review and Meta-Analysis of Randomised, Other-than-Placebo Controlled, Trials of Individualised Homeopathic Treatment

Robert T. Mathie

¹Homeopathy Research Institute, London, United Kingdom

,

Susanne Ulbrich-Zürni

²Department of Research, Swiss Homeopathy Association, Zürich, Switzerland

,

Petter Viksveen

³Faculty of Health Sciences, University of Stavanger, Stavanger, Norway

,

E. Rachel Roberts

¹Homeopathy Research Institute, London, United Kingdom

,

Elizabeth S. Baitson

¹Homeopathy Research Institute, London, United Kingdom

,

Lynn A. Legg

⁴Department of Biomedical Engineering, University of Strathclyde, Glasgow, United Kingdom

,

Jonathan R. T. Davidson

⁵Department of Psychiatry and Behavioral Science, Duke University Medical Center, Durham, North Carolina, United States

› Author Affiliations

Abstract

Background This study focuses on randomised controlled trials (RCTs) of individualised homeopathic treatment (IHT) in which the control (comparator) group was other than placebo (OTP).

Aims To determine the comparative effectiveness of IHT on health-related outcomes in adults and children for any clinical condition that has been the subject of at least one OTP-controlled trial. For each study, to assess the risk of bias and to determine whether its study attitude was predominantly ‘pragmatic’ or ‘explanatory’.

Methods Systematic review. For each eligible trial, published in the peer-reviewed literature up to the end of 2015, we assessed its risk of bias (internal validity) using the seven-domain Cochrane tool, and its relative pragmatic or explanatory attitude (external validity) using the 10-domain PRECIS tool. We grouped RCTs by whether they examined IHT as an alternative treatment (study design Ia), adjunctively with another intervention (design Ib), or compared with a no-intervention group (design II). For each RCT, we identified a ‘main outcome measure’ to use in meta-analysis: ‘relative effect size’ was reported as odds ratio (OR; values >1 favouring homeopathy) or standardised mean difference (SMD; values < 0 favouring homeopathy).

Results Eleven RCTs, representing 11 different medical conditions, were eligible for study. Five of the RCTs (four of which in design Ib) were judged to have pragmatic study attitude, two were explanatory, and four were equally pragmatic and explanatory. Ten trials were rated ‘high risk of bias’ overall: one of these, a pragmatic study with design Ib, had high risk of bias solely regarding participant blinding (a bias that is intrinsic to such trials); the other trial was rated ‘uncertain risk of bias’ overall. Eight trials had data that were extractable for analysis: for four heterogeneous trials with design Ia, the pooled OR was statistically non-significant; collectively for three clinically heterogeneous trials with design Ib, there was a statistically significant SMD favouring adjunctive IHT; in the remaining trial of design 1a, IHT was non-inferior to fluoxetine in the treatment of depression.

Conclusions Due to the low quality, the small number and the heterogeneity of studies, the current data preclude a decisive conclusion about the comparative effectiveness of IHT. Generalisability of findings is limited by the variable external validity identified overall; the most pragmatic study attitude was associated with RCTs of adjunctive IHT. Future OTP-controlled trials in homeopathy should aim, as far as possible, to promote both internal validity and external validity.

Keywords

comparative effectiveness - explanatory trial - individualised homeopathic treatment - meta-analysis - pragmatic trial - randomised controlled trial - risk of bias - systematic review

Full Text

References

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Supplementary Material

Supplementary Material