Evidence for novel susceptibility genes for late-onset Alzheimer's disease from a genome-wide association study of putative functional variants

doi:10.1093/hmg/ddm031

Human Molecular Genetics Advance Access originally published online on February 22, 2007
Human Molecular Genetics 2007 16(8):865-873; doi:10.1093/hmg/ddm031

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Evidence for novel susceptibility genes for late-onset Alzheimer's disease from a genome-wide association study of putative functional variants

Andrew Grupe¹^,*, Richard Abraham², Yonghong Li¹, Charles Rowland¹, Paul Hollingworth², Angharad Morgan², Luke Jehu², Ricardo Segurado², David Stone³, Eric Schadt³, Maha Karnoub³, Petra Nowotny⁴^,5^,6, Kristina Tacey¹, Joseph Catanese¹, John Sninsky¹, Carol Brayne⁷^,8, David Rubinsztein⁷^,8, Michael Gill⁹^,10, Brian Lawlor⁹^,10, Simon Lovestone¹¹, Peter Holmans², Michael O'Donovan², John C. Morris⁴^,5^,6, Leon Thal¹², Alison Goate⁴^,5^,6, Michael J. Owen² and Julie Williams²^,*

¹ Celera Diagnostics, 1401 Harbor Bay Parkway, Alameda, CA 94502, USA, ² Department of Psychological Medicine and Biostatistics and Bioinformatics Unit, Wales School of Medicine, Cardiff University, Heath Park, Cardiff CF14 4XN, UK, ³ Rosetta Inpharmatics, 401 Terry Avenue North, Seattle, WA 98109, USA, ⁴ Department of Psychiatry, ⁵ Department of Neurology and ⁶ Department of Genetics, Washington University School of Medicine, St Louis, MO 63110, USA, ⁷ Department of Public Health and Primary Care and ⁸ Department of Medical Genetics, Cambridge University, Cambridge CB2 2XY, UK, ⁹ Department of Psychiatry and ¹⁰ Institute of Neurology, Trinity College, Dublin 8, Ireland, ¹¹ Department of Neuroscience, Institute of Psychiatry King's College London, London SE5 8AF, UK and ¹² Department of Neurosciences, University of California, San Diego, La Jolla, CA 92093, USA

^* To whom correspondence should be addressed. Tel: +1 2920743247; Fax: +1 2920746554; Email: williamsj{at}cardiff.ac.uk or andrew.grupe{at}celeradiagnostics.com

Received November 1, 2006; Revised January 12, 2007; Accepted February 14, 2007

This study sets out to identify novel susceptibility genes forlate-onset Alzheimer's disease (LOAD) in a powerful set of samplesfrom the UK and USA (1808 LOAD cases and 2062 controls). Allelefrequencies of 17 343 gene-based putative functional singlenucleotide polymorphisms (SNPs) were tested for associationwith LOAD in a discovery case–control sample from theUK. A tiered strategy was used to follow-up significant variantsfrom the discovery sample in four independent sample sets. Here,we report the identification of several candidate SNPs thatshow significant association with LOAD. Three of the identifiedmarkers are located on chromosome 19 (meta-analysis: full sampleP = 6.94E – 81 to 0.0001), close to the APOE gene andexhibit linkage disequilibrium (LD) with the APOE ${varepsilon}$ 4 and ${varepsilon}$ 2/3 variants(0.09 < D'<1). Two of the three SNPs can be regarded asstudy-wide significant (expected number of false positives reachingthe observed significance level less than 0.05 per study). Sixteenadditional SNPs show evidence for association with LOAD [P =0.0010-0.00006; odds ratio (OR) = 1.07–1.45], severalof which map to known linkage regions, biological candidategenes and novel genes. Four SNPs not in LD with APOE show afalse positive rate of less than 2 per study, one of which showsstudy-wide suggestive evidence taking account of 17 343tests. This is a missense mutation in the galanin-like peptideprecursor gene (P = 0.00005, OR = 1.2, false positive rate =0.87).

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