GWAS of Longevity in CHARGE Consortium Confirms APOE and FOXO3 Candidacy

Linda Broer; AS Buchman; J Deelen; DS Evans; JD Faul; KL Lunetta; P Sebastiani; JA Smith; AV Smith; T Tanaka; L Yu; AM Arnold; T Aspelund; EJ Benjamin; PL De Jager; G Eirkisdottir; DA Evans; ME Garcia; Bert Hofman; RC Kaplan; SLR Kardia; DP Kiel; Ben Oostra; ES Orwoll; N Parimi; BM Psaty; Fernando Rivadeneira; JI Rotter; S Seshadri; A Singleton; Henning Tiemeier; André Uitterlinden; W Zhao; S Bandinelli; DA Bennett; L Ferrucci; V Gudnason; TB Harris; D Karasik; LJ Launer; TT Perls; PE (Eline) Slagboom; GJ Tranah; DR Weir; AB Newman; Cornelia Duijn; JM Murabito

doi:10.1093/gerona/glu166

GWAS of Longevity in CHARGE Consortium Confirms APOE and FOXO3 Candidacy

Linda Broer, AS Buchman, J Deelen, DS Evans, JD Faul, KL Lunetta, P Sebastiani, JA Smith, AV Smith, T Tanaka, L Yu, AM Arnold, T Aspelund, EJ Benjamin, PL De Jager, G Eirkisdottir, DA Evans, ME Garcia, Bert Hofman, RC KaplanSLR Kardia, DP Kiel, Ben Oostra, ES Orwoll, N Parimi, BM Psaty, Fernando Rivadeneira, JI Rotter, S Seshadri, A Singleton, Henning Tiemeier, André Uitterlinden, W Zhao, S Bandinelli, DA Bennett, L Ferrucci, V Gudnason, TB Harris, D Karasik, LJ Launer, TT Perls, PE (Eline) Slagboom, GJ Tranah, DR Weir, AB Newman, Cornelia Duijn, JM Murabito

Research output: Contribution to journal › Article › Academic › peer-review

223 Citations (Scopus)

Abstract

Background. The genetic contribution to longevity in humans has been estimated to range from 15% to 25%. Only two genes, APOE and FOXO3, have shown association with longevity in multiple independent studies. Methods. We conducted a meta-analysis of genome-wide association studies including 6,036 longevity cases, age >= 90 years, and 3,757 controls that died between ages 55 and 80 years. We additionally attempted to replicate earlier identified single nucleotide polymorphism (SNP) associations with longevity. Results. In our meta-analysis, we found suggestive evidence for the association of SNPs near CADM2 (odds ratio [OR] = 0.81; p value = 9.66 x 10(-7)) and GRIK2 (odds ratio = 1.24; p value = 5.09 x 10(-8)) with longevity. When attempting to replicate findings earlier identified in genome-wide association studies, only the APOE locus consistently replicated. In an additional look-up of the candidate gene FOXO3, we found that an earlier identified variant shows a highly significant association with longevity when including published data with our meta-analysis (odds ratio = 1.17; p value = 1.85 x 10(-10)). Conclusions. We did not identify new genome-wide significant associations with longevity and did not replicate earlier findings except for APOE and FOXO3. Our inability to find new associations with survival to ages >= 90 years because longevity represents multiple complex traits with heterogeneous genetic underpinnings, or alternatively, that longevity may be regulated by rare variants that are not captured by standard genome-wide genotyping and imputation of common variants.

Original language	Undefined/Unknown
Pages (from-to)	110-118
Number of pages	9
Journal	Journals of Gerontology Series A-Biological Sciences and Medical Sciences
Volume	70
Issue number	1
DOIs	https://doi.org/10.1093/gerona/glu166
Publication status	Published - 2015

Research programs

EMC MM-01-39-09-A
EMC NIHES-01-64-02
EMC NIHES-04-55-01

Access to Document

10.1093/gerona/glu166

Cite this

Broer, L., Buchman, AS., Deelen, J., Evans, DS., Faul, JD., Lunetta, KL., Sebastiani, P., Smith, JA., Smith, AV., Tanaka, T., Yu, L., Arnold, AM., Aspelund, T., Benjamin, EJ., De Jager, PL., Eirkisdottir, G., Evans, DA., Garcia, ME., Hofman, B., ... Murabito, JM. (2015). GWAS of Longevity in CHARGE Consortium Confirms APOE and FOXO3 Candidacy. Journals of Gerontology Series A-Biological Sciences and Medical Sciences, 70(1), 110-118. https://doi.org/10.1093/gerona/glu166

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title = "GWAS of Longevity in CHARGE Consortium Confirms APOE and FOXO3 Candidacy",

abstract = "Background. The genetic contribution to longevity in humans has been estimated to range from 15% to 25%. Only two genes, APOE and FOXO3, have shown association with longevity in multiple independent studies. Methods. We conducted a meta-analysis of genome-wide association studies including 6,036 longevity cases, age >= 90 years, and 3,757 controls that died between ages 55 and 80 years. We additionally attempted to replicate earlier identified single nucleotide polymorphism (SNP) associations with longevity. Results. In our meta-analysis, we found suggestive evidence for the association of SNPs near CADM2 (odds ratio [OR] = 0.81; p value = 9.66 x 10(-7)) and GRIK2 (odds ratio = 1.24; p value = 5.09 x 10(-8)) with longevity. When attempting to replicate findings earlier identified in genome-wide association studies, only the APOE locus consistently replicated. In an additional look-up of the candidate gene FOXO3, we found that an earlier identified variant shows a highly significant association with longevity when including published data with our meta-analysis (odds ratio = 1.17; p value = 1.85 x 10(-10)). Conclusions. We did not identify new genome-wide significant associations with longevity and did not replicate earlier findings except for APOE and FOXO3. Our inability to find new associations with survival to ages >= 90 years because longevity represents multiple complex traits with heterogeneous genetic underpinnings, or alternatively, that longevity may be regulated by rare variants that are not captured by standard genome-wide genotyping and imputation of common variants.",

author = "Linda Broer and AS Buchman and J Deelen and DS Evans and JD Faul and KL Lunetta and P Sebastiani and JA Smith and AV Smith and T Tanaka and L Yu and AM Arnold and T Aspelund and EJ Benjamin and {De Jager}, PL and G Eirkisdottir and DA Evans and ME Garcia and Bert Hofman and RC Kaplan and SLR Kardia and DP Kiel and Ben Oostra and ES Orwoll and N Parimi and BM Psaty and Fernando Rivadeneira and JI Rotter and S Seshadri and A Singleton and Henning Tiemeier and Andr{\'e} Uitterlinden and W Zhao and S Bandinelli and DA Bennett and L Ferrucci and V Gudnason and TB Harris and D Karasik and LJ Launer and TT Perls and Slagboom, {PE (Eline)} and GJ Tranah and DR Weir and AB Newman and Cornelia Duijn and JM Murabito",

year = "2015",

doi = "10.1093/gerona/glu166",

language = "Undefined/Unknown",

volume = "70",

pages = "110--118",

journal = "Journals of Gerontology Series A-Biological Sciences and Medical Sciences",

issn = "1079-5006",

publisher = "Oxford University Press",

number = "1",

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Broer, L, Buchman, AS, Deelen, J, Evans, DS, Faul, JD, Lunetta, KL, Sebastiani, P, Smith, JA, Smith, AV, Tanaka, T, Yu, L, Arnold, AM, Aspelund, T, Benjamin, EJ, De Jager, PL, Eirkisdottir, G, Evans, DA, Garcia, ME, Hofman, B, Kaplan, RC, Kardia, SLR, Kiel, DP, Oostra, B, Orwoll, ES, Parimi, N, Psaty, BM, Rivadeneira, F, Rotter, JI, Seshadri, S, Singleton, A, Tiemeier, H, Uitterlinden, A, Zhao, W, Bandinelli, S, Bennett, DA, Ferrucci, L, Gudnason, V, Harris, TB, Karasik, D, Launer, LJ, Perls, TT, Slagboom, PE, Tranah, GJ, Weir, DR, Newman, AB, Duijn, C & Murabito, JM 2015, 'GWAS of Longevity in CHARGE Consortium Confirms APOE and FOXO3 Candidacy', Journals of Gerontology Series A-Biological Sciences and Medical Sciences, vol. 70, no. 1, pp. 110-118. https://doi.org/10.1093/gerona/glu166

TY - JOUR

T1 - GWAS of Longevity in CHARGE Consortium Confirms APOE and FOXO3 Candidacy

AU - Broer, Linda

AU - Buchman, AS

AU - Deelen, J

AU - Evans, DS

AU - Faul, JD

AU - Lunetta, KL

AU - Sebastiani, P

AU - Smith, JA

AU - Smith, AV

AU - Tanaka, T

AU - Yu, L

AU - Arnold, AM

AU - Aspelund, T

AU - Benjamin, EJ

AU - De Jager, PL

AU - Eirkisdottir, G

AU - Evans, DA

AU - Garcia, ME

AU - Hofman, Bert

AU - Kaplan, RC

AU - Kardia, SLR

AU - Kiel, DP

AU - Oostra, Ben

AU - Orwoll, ES

AU - Parimi, N

AU - Psaty, BM

AU - Rivadeneira, Fernando

AU - Rotter, JI

AU - Seshadri, S

AU - Singleton, A

AU - Tiemeier, Henning

AU - Uitterlinden, André

AU - Zhao, W

AU - Bandinelli, S

AU - Bennett, DA

AU - Ferrucci, L

AU - Gudnason, V

AU - Harris, TB

AU - Karasik, D

AU - Launer, LJ

AU - Perls, TT

AU - Slagboom, PE (Eline)

AU - Tranah, GJ

AU - Weir, DR

AU - Newman, AB

AU - Duijn, Cornelia

AU - Murabito, JM

PY - 2015

Y1 - 2015

N2 - Background. The genetic contribution to longevity in humans has been estimated to range from 15% to 25%. Only two genes, APOE and FOXO3, have shown association with longevity in multiple independent studies. Methods. We conducted a meta-analysis of genome-wide association studies including 6,036 longevity cases, age >= 90 years, and 3,757 controls that died between ages 55 and 80 years. We additionally attempted to replicate earlier identified single nucleotide polymorphism (SNP) associations with longevity. Results. In our meta-analysis, we found suggestive evidence for the association of SNPs near CADM2 (odds ratio [OR] = 0.81; p value = 9.66 x 10(-7)) and GRIK2 (odds ratio = 1.24; p value = 5.09 x 10(-8)) with longevity. When attempting to replicate findings earlier identified in genome-wide association studies, only the APOE locus consistently replicated. In an additional look-up of the candidate gene FOXO3, we found that an earlier identified variant shows a highly significant association with longevity when including published data with our meta-analysis (odds ratio = 1.17; p value = 1.85 x 10(-10)). Conclusions. We did not identify new genome-wide significant associations with longevity and did not replicate earlier findings except for APOE and FOXO3. Our inability to find new associations with survival to ages >= 90 years because longevity represents multiple complex traits with heterogeneous genetic underpinnings, or alternatively, that longevity may be regulated by rare variants that are not captured by standard genome-wide genotyping and imputation of common variants.

AB - Background. The genetic contribution to longevity in humans has been estimated to range from 15% to 25%. Only two genes, APOE and FOXO3, have shown association with longevity in multiple independent studies. Methods. We conducted a meta-analysis of genome-wide association studies including 6,036 longevity cases, age >= 90 years, and 3,757 controls that died between ages 55 and 80 years. We additionally attempted to replicate earlier identified single nucleotide polymorphism (SNP) associations with longevity. Results. In our meta-analysis, we found suggestive evidence for the association of SNPs near CADM2 (odds ratio [OR] = 0.81; p value = 9.66 x 10(-7)) and GRIK2 (odds ratio = 1.24; p value = 5.09 x 10(-8)) with longevity. When attempting to replicate findings earlier identified in genome-wide association studies, only the APOE locus consistently replicated. In an additional look-up of the candidate gene FOXO3, we found that an earlier identified variant shows a highly significant association with longevity when including published data with our meta-analysis (odds ratio = 1.17; p value = 1.85 x 10(-10)). Conclusions. We did not identify new genome-wide significant associations with longevity and did not replicate earlier findings except for APOE and FOXO3. Our inability to find new associations with survival to ages >= 90 years because longevity represents multiple complex traits with heterogeneous genetic underpinnings, or alternatively, that longevity may be regulated by rare variants that are not captured by standard genome-wide genotyping and imputation of common variants.

U2 - 10.1093/gerona/glu166

DO - 10.1093/gerona/glu166

M3 - Article

C2 - 25199915

SN - 1079-5006

VL - 70

SP - 110

EP - 118

JO - Journals of Gerontology Series A-Biological Sciences and Medical Sciences

JF - Journals of Gerontology Series A-Biological Sciences and Medical Sciences

IS - 1

ER -