Affiliations: [a] Dementia Research Group, School of Clinical Sciences, University of Bristol, Frenchay Day Hospital, Bristol, UK | [b] School of Experimental Psychology, University of Bristol, Clifton, UK
Correspondence:
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Correspondence to: Patrick G. Kehoe, Dementia Research Group, School of Clinical Sciences, University of Bristol Frenchay Day Hospital, Bristol, BS16 1LE, United Kingdom. Tel.: +44 117 340 3070; E-mail: Patrick.Kehoe@bristol.ac.uk.
Note: [1] These authors contributed equally to this work.
Abstract: Vascular cognitive impairment (VCI), including vascular dementia, is the second most common dementia after Alzheimer's disease. Despite its prevalence, the genetic etiology of sporadic VCI is largely unknown. We conducted a systematic review of all published genetic association studies of forms of sporadic VCI prior to 6 July 2012. An initial pool of 229 gene association studies yielded 104 papers (72 polymorphisms from 47 genes) that met inclusion criteria for analysis. Systematic meta-analysis was conducted on 6 polymorphisms (which had 3 or more published case-control cohorts from 69 papers) in the APOE, ACT, ACE, MTHFR, PON1, and PSEN-1 genes. Associations of increased risk for VCI were found for APOE ε4 (1.818 (95% CI = 1.611–2.053), p < 0.001; n = 3,554 cases, n = 12,277 controls) and MTHFR rs1801133 (1.323 (95% CI = 1.061–1.650) p = 0.013); n = 659 cases, n = 981 controls). There was marginal evidence of a protective effect for APOE ε2 (0.885 (95% CI = 0.783–0.999), p = 0.048; n = 3,320 cases, n = 10,786 controls). This systematic study of all published genetic association studies of sporadic VCI supports MTHFR and APOE as susceptibility genes for VCI. It also shows the utility of meta-analysis as a tool to identify potential candidate genes from numerous individual small-scale studies of diseases where sample recruitment may be limited for a variety of practical reasons.
