Good laboratory practice: preventing introduction of bias at the bench

Malcolm R Macleod; Marc Fisher; Victoria O'Collins; Emily S Sena; Ulrich Dirnagl; Philip M W Bath; Alistair Buchan; H Bart van der Worp; Richard Traystman; Kazuo Minematsu; Geoffrey A Donnan; David W Howells

doi:10.1161/STROKEAHA.108.525386

Good laboratory practice: preventing introduction of bias at the bench

Stroke. 2009 Mar;40(3):e50-2. doi: 10.1161/STROKEAHA.108.525386. Epub 2008 Aug 14.

Authors

Malcolm R Macleod¹, Marc Fisher, Victoria O'Collins, Emily S Sena, Ulrich Dirnagl, Philip M W Bath, Alistair Buchan, H Bart van der Worp, Richard Traystman, Kazuo Minematsu, Geoffrey A Donnan, David W Howells

Affiliation

¹ Centre for Clinical Brain Sciences, University of Edinburgh, UK.

PMID: 18703798
DOI: 10.1161/STROKEAHA.108.525386

Abstract

Background and purpose: As a research community, we have failed to demonstrate that drugs which show substantial efficacy in animal models of cerebral ischemia can also improve outcome in human stroke. Summary of Review- Accumulating evidence suggests this may be due, at least in part, to problems in the design, conduct and reporting of animal experiments which create a systematic bias resulting in the overstatement of neuroprotective efficacy.

Conclusions: Here, we set out a series of measures to reduce bias in the design, conduct and reporting of animal experiments modeling human stroke.

MeSH terms

Animals
Bias*
Conflict of Interest
Disease Models, Animal
Drug Industry
Humans
Random Allocation
Research Design / standards*
Research Support as Topic
Sample Size
Stroke / drug therapy*
Treatment Outcome