Genome-wide association meta-analysis of human longevity identifies a novel locus conferring survival beyond 90 years of age

Deelen, Joris; Beekman, Marian; Uh, Hae‐Won; Broer, Linda; Ayers, Kristin L.; Tan, Qihua; Kamatani, Yoichiro; Bennet, Anna M.; Tamm, Riin; Trompet, Stella; Guðbjartsson, Daníel F.; Flachsbart, Friederike; Rose, Giuseppina; Viktorin, Alexander; Fischer, Krista; Nygaard, Marianne; Cordell, Heather J.; Crocco, Paolina; Akker, Erik B. van den; Böhringer, Stefan; Helmer, Quinta; Nelson, Christopher P.; Saunders, Gary; Alver, Maris; Andersen‐Ranberg, Karen; Breen, Marie E.; Breggen, Ruud van der; Caliebe, Amke; Capri, Miriam; Cevenini, Elisa; Collerton, Joanna; Dato, Serena; Davies, Karen; Ford, Ian; Gampe, Jutta; Garagnani, Paolo; Geus, Eco J. C. de; Harrow, Jennifer; Heemst, Diana van; Heijmans, Bastiaan T.; Heinsen, Femke-Anouska; Hottenga, Jouke‐Jan; Hofman, Albert; Jeune, Bernard; Jónsson, Pálmi V.; Lathrop, Mark; Lechner, Doris; Martin-Ruiz, Carmen; McNerlan, Susan E.; Mihailov, Evelin; Montesanto, Alberto; Mooijaart, Simon P.; Murphy, Anne M.; Nøhr, Ellen Aagaard; Paternoster, Lavinia; Postmus, Iris; Rivadeneira, Fernando; Ross, Owen A.; Salvioli, Stefano; Sattar, Naveed; Schreiber, Stefan; Stefánsson, Hreinn; Stott, David J.; Tiemeier, Henning; Uitterlinden, André G.; Westendorp, Rudi G.J.; Willemsen, Gonneke; Samani, Nilesh J.; Galán, Pilar; Sørensen, Thorkild I A; Boomsma, Dorret I.; Jukema, J. Wouter; Rea, Irene Maeve; Passarino, Giuseppe; Craen, Anton J. M. de; Christensen, Kaare; Nebel, Almut; Stefánsson, Kāri; Metspalu, Andres; Magnusson, Patrik K. E.; Blanché, Hélène; Christiansen, Lene; Kirkwood, Thomas B. L.; Duijn, Cornelia M. van; Franceschi, Claudio; Houwing-Duistermaat, Jeanine J.; Slagboom, P. Eline

doi:10.1093/hmg/ddu139

Cited by 231 publications

(242 citation statements)

References 49 publications

Supporting

Mentioning

226

Contrasting

Unclassified

Order By: Relevance

“…In the DKLS, DNA was isolated from whole blood using standard methods (Miller et al ., 1988) and genotyping was carried out according to the manufacturer's protocol using the Illumina HumanOmniExpress BeadChips (Illumina Inc.) (Deelen et al ., 2014), which contains 730 525 SNP markers with a median spacing of 2.1 kb and a mean spacing of 4.0 kb.…”

Section: Methodsmentioning

confidence: 99%

See 1 more Smart Citation

Copy number variation associates with mortality in long‐lived individuals: a genome‐wide assessment

et al. 2015

Self Cite

View full text Add to dashboard Cite

SummaryCopy number variants (CNVs) represent a significant source of genetic variation in the human genome and have been implicated in numerous diseases and complex traits. To date, only a few studies have investigated the role of CNVs in human lifespan. To investigate the impact of CNVs on prospective mortality at the extreme end of life, where the genetic component of lifespan appears most profound, we analyzed genomewide CNV data in 603 Danish nonagenarians and centenarians (mean age 96.9 years, range 90.0–102.5 years). Replication was performed in 500 long‐lived individuals from the Leiden Longevity Study (mean age 93.2 years, range 88.9–103.4 years). First, we assessed the association between the CNV burden of each individual (the number of CNVs, the average CNV length, and the total CNV length) and mortality and found a significant increase in mortality per 10 kb increase in the average CNV length, both for all CNVs (hazard ratio (HR) = 1.024, P = 0.002) and for duplications (HR = 1.011, P = 0.005), as well as per 100 kb increase in the total length of deletions (HR = 1.009, P = 0.0005). Next, we assessed the relation between specific deletions and duplications and mortality. Although no genome–wide significant associations were discovered, we identified six deletions and one duplication that showed consistent association with mortality in both or either of the sexes across both study populations. These results indicate that the genome–wide CNV burden, specifically the average CNV length and the total CNV length, associates with higher mortality in long‐lived individuals.

show abstract

Section: Methodsmentioning

confidence: 99%

“…So far, only a limited number of loci have been consistently associated with length of life (Murabito et al ., 2012; Deelen et al ., 2014), and hence much of the heritability is still unaccounted for. This missing heritability might in part be explained by copy number variants (CNVs) (Manolio et al ., 2009).…”

Section: Introductionmentioning

confidence: 99%

Copy number variation associates with mortality in long‐lived individuals: a genome‐wide assessment

et al. 2015

Self Cite

View full text Add to dashboard Cite

show abstract

“…GWAS of human longevity in worldwide samples (North America, Europe and very recently China) generally failed to give new insights into genetic determinants of human longevity: only the TOMM40/APOE/APOC1 locus, associated with longevity, was replicated in different populations (Deelen et al., 2014; Lin et al., 2016; Newman et al., 2010; Sebastiani et al., 2012), while rs2149954 on 5q33.3 (Deelen et al., 2014; Zeng et al., 2016) and the FOXO3A locus (Broer et al., 2015 and references therein) are the other signals showing population‐specific associations. Some authors attempted to analyse epistatic intragenic (Tan, Soerensen, Kruse, Christensen & Christiansen, 2013; Zeng et al., 2010) or intergenic effects (Napolioni, Giannì, Carpi, Predazzi & Lucarini, 2011a; Napolioni et al., 2011b), however comprising a limited number of genetic variants.…”

Section: Introductionmentioning

confidence: 99%

The genetic component of human longevity: New insights from the analysis of pathway‐based SNP‐SNP interactions

et al. 2018

Self Cite

View full text Add to dashboard Cite

SummaryIn human longevity studies, single nucleotide polymorphism (SNP) analysis identified a large number of genetic variants with small effects, yet not easily replicable in different populations. New insights may come from the combined analysis of different SNPs, especially when grouped by metabolic pathway. We applied this approach to study the joint effect on longevity of SNPs belonging to three candidate pathways, the insulin/insulin‐like growth factor signalling (IIS), DNA repair and pro/antioxidant. We analysed data from 1,058 tagging SNPs in 140 genes, collected in 1825 subjects (1,089 unrelated nonagenarians from the Danish 1905 Birth Cohort Study and 736 Danish controls aged 46–55 years) for evaluating synergic interactions by SNPsyn. Synergies were further tested by the multidimensional reduction (MDR) approach, both intra‐ and interpathways. The best combinations (FDR<0.0001) resulted those encompassing IGF1R‐rs12437963 and PTPN1‐rs6067484, TP53‐rs2078486 and ERCC2‐rs50871, TXNRD1‐rs17202060 and TP53‐rs2078486, the latter two supporting a central role of TP53 in mediating the concerted activation of the DNA repair and pro‐antioxidant pathways in human longevity. Results were consistently replicated with both approaches, as well as a significant effect on longevity was found for the GHSR gene, which also interacts with partners belonging to both IIS and DNA repair pathways (PAPPA,PTPN1,PARK7, MRE11A). The combination GHSR‐MREA11, positively associated with longevity by MDR, was further found influencing longitudinal survival in nonagenarian females (p = .026). Results here presented highlight the validity of SNP‐SNP interactions analyses for investigating the genetics of human longevity, confirming previously identified markers but also pointing to novel genes as central nodes of additional networks involved in human longevity.

show abstract

“…APOE and FOXO3 were initially detected in candidate‐driven case–control investigations, but APOE has since then been confirmed in a number of genome‐wide association studies (GWAS). In addition, a single nucleotide polymorphism (SNP) on chromosome 5q33.3 was recently identified in a GWAS meta‐analysis on long‐lived individuals (LLI) aged ≥ 90 years (Deelen et al ., 2014). Besides the detection of APOE and the 5q33.3 locus, longevity GWAS have been relatively unsuccessful and have failed to reveal novel associations with genome‐wide significance or sufficient reproducibility (Deelen et al ., 2011, 2014; Nebel et al ., 2011).…”

mentioning

confidence: 99%

“…In addition, a single nucleotide polymorphism (SNP) on chromosome 5q33.3 was recently identified in a GWAS meta‐analysis on long‐lived individuals (LLI) aged ≥ 90 years (Deelen et al ., 2014). Besides the detection of APOE and the 5q33.3 locus, longevity GWAS have been relatively unsuccessful and have failed to reveal novel associations with genome‐wide significance or sufficient reproducibility (Deelen et al ., 2011, 2014; Nebel et al ., 2011). Here, we performed a large‐scale candidate gene study by targeting established immune‐associated loci present on the Immunochip (Trynka et al ., 2011).…”

mentioning

confidence: 99%

Immunochip analysis identifies association of the RAD 50/ IL 13 region with human longevity

et al. 2016

Self Cite

View full text Add to dashboard Cite

SummaryHuman longevity is characterized by a remarkable lack of confirmed genetic associations. Here, we report on the identification of a novel locus for longevity in the RAD50/IL13 region on chromosome 5q31.1 using a combined European sample of 3208 long‐lived individuals (LLI) and 8919 younger controls. First, we performed a large‐scale association study on 1458 German LLI (mean age 99.0 years) and 6368 controls (mean age 57.2 years) by targeting known immune‐associated loci covered by the Immunochip. The analysis of 142 136 autosomal single nucleotide polymorphisms (SNPs) revealed an Immunochip‐wide significant signal (PI mmunochip = 7.01 × 10–9) for the SNP rs2075650 in the TOMM40/APOE region, which has been previously described in the context of human longevity. To identify novel susceptibility loci, we selected 15 markers with PI mmunochip < 5 × 10–4 for replication in two samples from France (1257 LLI, mean age 102.4 years; 1811 controls, mean age 49.1 years) and Denmark (493 LLI, mean age 96.2 years; 740 controls, mean age 63.1 years). The association at SNP rs2706372 replicated in the French study collection and showed a similar trend in the Danish participants and was also significant in a meta‐analysis of the combined French and Danish data after adjusting for multiple testing. In a meta‐analysis of all three samples, rs2706372 reached a P‐value of PI mmunochip+Repl = 5.42 × 10−7 (OR = 1.20; 95% CI = 1.12–1.28). SNP rs2706372 is located in the extended RAD50/IL13 region. RAD50 seems a plausible longevity candidate due to its involvement in DNA repair and inflammation. Further studies are needed to identify the functional variant(s) that predispose(s) to a long and healthy life.

show abstract

Genome-wide association meta-analysis of human longevity identifies a novel locus conferring survival beyond 90 years of age

Cited by 231 publications

References 49 publications

Copy number variation associates with mortality in long‐lived individuals: a genome‐wide assessment

Copy number variation associates with mortality in long‐lived individuals: a genome‐wide assessment

The genetic component of human longevity: New insights from the analysis of pathway‐based SNP‐SNP interactions

Immunochip analysis identifies association of the RAD 50/ IL 13 region with human longevity

Contact Info

Product

Resources

About