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author Benitez, Bruno A.
Jin, Sheng Chih
Guerreiro, Rita
Graham, Rob
Lord, Jenny
Harold, Denise
Sims, Rebecca
Lambert, Jean-Charles
Gibbs, J. Raphael
Bras, Jose
Sassi, Celeste
Harari, Oscar
Bertelsen, Sarah
Lupton, Michelle K.
Powell, John
Bellenguez, Celine
Brown, Kristelle
Medway, Christopher
Haddick, Patrick CG.
van der Brug, Marcel P.
Bhangale, Tushar
Ortmann, Ward
Behrens, Tim
Mayeux, Richard
Pericak-Vance, Margaret A.
Farrer, Lindsay A.
Schellenberg, Gerard D.
Haines, Jonathan L.
Turton, Jim
Braae, Anne
Barber, Imelda
Fagan, Anne M.
Holtzman, David M.
Morris, John C.
Williams, Julie
Kauwe, John S.K.
Amouyel, Philippe
Morgan, Kevin
Singleton, Andy
Hardy, John
Goate, Alison M.
Cruchaga, Carlos
author_facet Benitez, Bruno A.
Jin, Sheng Chih
Guerreiro, Rita
Graham, Rob
Lord, Jenny
Harold, Denise
Sims, Rebecca
Lambert, Jean-Charles
Gibbs, J. Raphael
Bras, Jose
Sassi, Celeste
Harari, Oscar
Bertelsen, Sarah
Lupton, Michelle K.
Powell, John
Bellenguez, Celine
Brown, Kristelle
Medway, Christopher
Haddick, Patrick CG.
van der Brug, Marcel P.
Bhangale, Tushar
Ortmann, Ward
Behrens, Tim
Mayeux, Richard
Pericak-Vance, Margaret A.
Farrer, Lindsay A.
Schellenberg, Gerard D.
Haines, Jonathan L.
Turton, Jim
Braae, Anne
Barber, Imelda
Fagan, Anne M.
Holtzman, David M.
Morris, John C.
Williams, Julie
Kauwe, John S.K.
Amouyel, Philippe
Morgan, Kevin
Singleton, Andy
Hardy, John
Goate, Alison M.
Cruchaga, Carlos
author_sort Benitez, Bruno A.
collection PubMed
description 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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spelling pubmed-39615572015-04-09 Missense variant in TREML2 protects against Alzheimer's disease Benitez, Bruno A. Jin, Sheng Chih Guerreiro, Rita Graham, Rob Lord, Jenny Harold, Denise Sims, Rebecca Lambert, Jean-Charles Gibbs, J. Raphael Bras, Jose Sassi, Celeste Harari, Oscar Bertelsen, Sarah Lupton, Michelle K. Powell, John Bellenguez, Celine Brown, Kristelle Medway, Christopher Haddick, Patrick CG. van der Brug, Marcel P. Bhangale, Tushar Ortmann, Ward Behrens, Tim Mayeux, Richard Pericak-Vance, Margaret A. Farrer, Lindsay A. Schellenberg, Gerard D. Haines, Jonathan L. Turton, Jim Braae, Anne Barber, Imelda Fagan, Anne M. Holtzman, David M. Morris, John C. Williams, Julie Kauwe, John S.K. Amouyel, Philippe Morgan, Kevin Singleton, Andy Hardy, John Goate, Alison M. Cruchaga, Carlos Neurobiol Aging Genetic Report 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. Elsevier 2014-06 /pmc/articles/PMC3961557/ /pubmed/24439484 http://dx.doi.org/10.1016/j.neurobiolaging.2013.12.010 Text en © 2014 The Authors. Published by Elsevier Inc. https://creativecommons.org/licenses/by/3.0/ Open Access under CC BY 3.0 (https://creativecommons.org/licenses/by/3.0/) license
spellingShingle Genetic Report Abstract
Benitez, Bruno A.
Jin, Sheng Chih
Guerreiro, Rita
Graham, Rob
Lord, Jenny
Harold, Denise
Sims, Rebecca
Lambert, Jean-Charles
Gibbs, J. Raphael
Bras, Jose
Sassi, Celeste
Harari, Oscar
Bertelsen, Sarah
Lupton, Michelle K.
Powell, John
Bellenguez, Celine
Brown, Kristelle
Medway, Christopher
Haddick, Patrick CG.
van der Brug, Marcel P.
Bhangale, Tushar
Ortmann, Ward
Behrens, Tim
Mayeux, Richard
Pericak-Vance, Margaret A.
Farrer, Lindsay A.
Schellenberg, Gerard D.
Haines, Jonathan L.
Turton, Jim
Braae, Anne
Barber, Imelda
Fagan, Anne M.
Holtzman, David M.
Morris, John C.
Williams, Julie
Kauwe, John S.K.
Amouyel, Philippe
Morgan, Kevin
Singleton, Andy
Hardy, John
Goate, Alison M.
Cruchaga, Carlos
Missense variant in TREML2 protects against Alzheimer's disease
title Missense variant in TREML2 protects against Alzheimer's disease
title_full Missense variant in TREML2 protects against Alzheimer's disease
title_fullStr Missense variant in TREML2 protects against Alzheimer's disease
title_full_unstemmed Missense variant in TREML2 protects against Alzheimer's disease
title_short Missense variant in TREML2 protects against Alzheimer's disease
title_sort missense variant in treml2 protects against alzheimer's disease
topic Genetic Report Abstract
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3961557/
https://www.ncbi.nlm.nih.gov/pubmed/24439484
http://dx.doi.org/10.1016/j.neurobiolaging.2013.12.010
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