Missense variant in TREML2 protects against Alzheimer's disease

Bruno A Benitez,Lindsay A Farrer,J Raphael Gibbs,Marcel P Van Der Brug,Celeste Sassi,Christopher Medway,John C Morris,Kevin Morgan,Rob Graham,Sheng Chih Jin,Jenny Lord,Philippe Amouyel,Anne Braae,Denise Harold,Tushar Bhangale,Rebecca Sims,Alison M Goate,Tim Behrens,John Powell,Carlos Cruchaga,Kristelle Brown,Oscar Harari,Richard Mayeux,Andy Singleton,Jonathan L Haines,Imelda Barber,Julie Williams,Ward Ortmann,David M Holtzman,John Hardy,Michelle K Lupton,Anne M Fagan,Gerard D Schellenberg,Sarah Bertelsen,Rita Guerreiro,Jean‐Charles Lambert ,José Brás ,Céline Bellenguez ,John S K Kauwe ,James Turton ,Margaret A Pericak‐Vance ,Patrick C.g Haddick

doi:10.1016/j.neurobiolaging.2013.12.010

Abstract

TREM and TREM-like receptors are a structurally similar protein family encoded by genes clustered on chromosome 6p21.11. Recent studies have identified a rare coding variant (p.R47H) in TREM2 that confers a high risk for Alzheimer's disease (AD). In addition, common single nucleotide polymorphisms in this genomic region are associated with cerebrospinal fluid biomarkers for AD and a common intergenic variant found near the TREML2 gene has been identified to be protective for AD. However, little is known about the functional variant underlying the latter association or its relationship with the p.R47H. Here, we report comprehensive analyses using whole-exome sequencing data, cerebrospinal fluid biomarker analyses, meta-analyses (16,254 cases and 20,052 controls) and cell-based functional studies to support the role of the TREML2 coding missense variant p.S144G (rs3747742) as a potential driver of the meta-analysis AD-associated genome-wide association studies signal. Additionally, we demonstrate that the protective role of TREML2 in AD is independent of the role of TREM2 gene as a risk factor for AD.

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