Spontaneous brain microbleeds: systematic review, subgroup analyses and standards for study design and reporting

doi:10.1093/brain/awl387

Brain Advance Access originally published online on February 24, 2007
Brain 2007 130(8):1988-2003; doi:10.1093/brain/awl387

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Review Article

Spontaneous brain microbleeds: systematic review, subgroup analyses and standards for study design and reporting

Charlotte Cordonnier, Rustam Al-Shahi Salman and Joanna Wardlaw

Division of Clinical Neurosciences, Western General Hospital, University of Edinburgh, Edinburgh, UK

Correspondence to: Charlotte Cordonnier, Bramwell Dott Building, Division of Clinical Neurosciences, Western General Hospital, University of Edinburgh, Edinburgh EH4 2XU, UK E-mail: c-cordonnier{at}chru-lille.fr

Brain microbleeds (BMBs) are seen as small, homogeneous, roundfoci of low signal intensity on magnetic resonance imaging gradientecho (GRE) Formula sequences. BMBs might only be a biomarker for microangiopathy, or alternativelyBMBs might provide useful diagnostic and prognostic information,potentially with therapeutic implications for the treatmentof stroke. Because of the rapid expansion in recent BMB research,we systematically reviewed and critically appraised the publishedliterature according to QUADAS, STARD and Cochrane principles.Our selection criteria were met by 54 studies of 53 case seriesinvolving 9073 participants, 4432 of whom were people with cerebrovasculardiseases. There were significant biases in many of the studies:variation in MRI magnet strength, flip angle, slice gap andslice thickness; inconsistent definitions of BMB size (23% didnot define size at all, and of those that did 44% chose a diameterof $≤$ 5 mm); only 30% included participants who were representativeof the disease under study; and only 53% mentioned that BMBevaluation was blinded to other factors of interest. By poolingdata from similar studies, we found that the prevalence of BMBswas 5% [95% confidence interval (CI) 4–6] in healthy adults,34% (95% CI 31–36) in people with ischaemic stroke, and60% (95% CI 57–64) in people with non-traumatic intracerebralhaemorrhage (ICH). In the studies where a distinction couldbe made, BMBs were more prevalent among recurrent strokes thanfirst-ever strokes: they affected 23% (95% CI 18–29) withfirst-ever ischaemic stroke but 44% (95% CI 34–54) withrecurrent ischaemic stroke, and 52% (95% CI 47–56) withfirst-ever ICH but 83% (95% CI 71–90) with recurrent ICH.By pooling data that could be extracted from similar studies,it appears that BMBs are associated with hypertension (OR 3.9,95% CI 2.4–6.4) and diabetes mellitus (OR 2.2, 95% CI1.2–4.2) in otherwise healthy adults, and that they areassociated with hypertension (OR 2.3, 95% CI 1.7–3.0)in adults with cerebrovascular diseases. The association withhypertension was robust in sensitivity analyses. There is apressing need for better designed studies to assess the diagnosticutility of BMBs, disentangle the many likely influences on theiroccurrence, and determine their prognostic utility and whetherthey should influence treatment. We conclude by proposing criteriafor ideal study design and reporting.

Key Words: stroke; intracerebral haemorrhage; magnetic resonance imaging; microbleeds; epidemiology

Abbreviations: BMB, brain microbleeds; CADASIL, cerebral autosomal dominant arteriopathy with subcortical infarcts and leucoencephalopathy; CI, confidence interval; EPI, echo planar imaging; GRE, gradient echo; ICH, intracerebral haemorrhage; OR, odds ratio; QUADAS, Quality Assessment of Diagnostic Accuracy Studies; STARD, Standards for the Reporting of Diagnostic Accuracy; T, tesla; TIA, transient ischaemic attack; tPA, tissue plasminogen activator; TR, Relaxation Time; TE, Echo Time

Received October 12, 2006. Revised December 1, 2006. Accepted December 19, 2006.

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