Genome‐wide linkage analysis for human longevity: Genetics of Healthy Aging Study

Beekman, Marian; Blanché, Hélène; Perola, Markus; Hervonen, A.; Bezrukov, Vladislav; Sikora, Ewa; Flachsbart, Friederike; Christiansen, Lene; Craen, Anton J. M. de; Kirkwood, Tom; Rea, Irene Maeve; Poulain, Michel; Robine, Jean-Marie; Valensin, Silvana; Stazi, Maria Antonietta; Passarino, Giuseppe; Deiana, Luca; Gonos, Efstathios S.; Paternoster, Lavinia; Sørensen, Thorkild I A; Tan, Qihua; Helmer, Quinta; Akker, Erik B. van den; Deelen, Joris; Martella, Francesca; Cordell, Heather J.; Ayers, Kristin L.; Vaupel, James W.; Törnwall, Outi; Johnson, Thomas E.; Schreiber, Stefan; Lathrop, Mark; Skytthe, Axel; Westendorp, Rudi G.J.; Christensen, Kaare; Gampe, Jutta; Nebel, Almut; Houwing-Duistermaat, Jeanine J.; Slagboom, P. Eline; Franceschi, Claudio

doi:10.1111/acel.12039

Cited by 173 publications

(112 citation statements)

References 41 publications

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“…Our findings indicated that cognitive and functional parameters (SMMSE, ADL scale and hand grip strength), self-reported health and clinical parameters (haemoglobin, creatinine and total cholesterol) are associated in 90+ sib-ships. This analysis suggests that the GEHA familial/genetics model of healthy aging allowed us to observe that the cognitive and physical abilities, together with the above mentioned haematochemical parameters appear to be influenced by familiarity/genetics, which has been recently demonstrated to play a role in the longevity of the sib-ships we analysed (Beekman et al 2013). Remarkably, also the self-reported health resulted to be associated in 90+ siblings, showing that well-being runs along families.…”

Section: Discussionsupporting

confidence: 60%

“…It can be considered the first of other similar investigations, on the assumption that analogous micro-heterogeneity is present in the 90+ populations recruited in the other geographic areas which contributed to the GEHA project. Indeed, the results of the genome-wide linkage analysis suggest that the Northern and Southern Europe populations contributed differently to the identification of the four chromosomal regions associated with longevity (Beekman et al 2013). Thus, the present study can help in interpreting the genetic results obtained by the GEHA project whose major aim is the comprehensive evaluation of phenotypic and genetic data.…”

Section: Conclusion and Future Perspectivesmentioning

confidence: 71%

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Health status and 6 years survival of 552 90+ Italian sib-ships recruited within the EU Project GEHA (GEnetics of Healthy Ageing)

Cevenini¹,

Cotichini²,

Stazi³

et al. 2013

AGE

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In a scenario of increasing life expectancy worldwide, it is mandatory to identify the characteristics of a healthy aging phenotype, including survival predictors, and to disentangle those related to environment/ lifestyle versus those related to familiarity/genetics. To this aim we comprehensively characterised a cohort of 1,160 Italian subjects of 90 years and over (90+, mean age 93 years; age range 90-106 years) followed for 6 years survival, belonging to 552 sib-ships (familiar longevity) recruited (2005)(2006)(2007)(2008) within the EU-funded GEHA project in three Italian geographic areas (Northern, Central and Southern Italy) different for urban/rural and socio-economical characteristics. On the whole, the following factors emerged as significant predictors of survival after 90 years of age: absence of cognitive impairment and physical disability, high hand grip strength scores and body mass index (BMI) values, "excellent/good" self-reported health, high haemoglobin and total cholesterol levels and low creatinine levels. These parameters, excluding BMI values, were also significantly associated within sib-ships, suggesting a strong familial/genetic component. Geographical micro-heterogeneity of survival predictors emerged, such as functional and physical status being more important in Southern than in Central and Northern Italy. In conclusion, we identified modifiable survival predictors related to specific domains, whose role and importance vary according to the geographic area considered and which can help in interpreting the genetic results obtained by the GEHA project, whose major aim is the comprehensive evaluation of phenotypic and genetic data.

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Section: Discussionsupporting

confidence: 60%

Section: Conclusion and Future Perspectivesmentioning

confidence: 71%

Health status and 6 years survival of 552 90+ Italian sib-ships recruited within the EU Project GEHA (GEnetics of Healthy Ageing)

Cevenini¹,

Cotichini²,

Stazi³

et al. 2013

AGE

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show abstract

“…Recent data also support an association of ApoE and mortality in long-lived individuals. A genome-wide linkage analysis with nonagenarians identified ApoE as a longevity gene (Beekman et al, 2013), which is in agreement with the results of a recent case-control genome-wide association study comparing long-lived individuals (mean age: 99.7 years) and Experimental Gerontology 53 (2014) [16][17][18][19][20][21][22][23] younger controls from Germany (Nebel et al, 2011). However, whether ApoE influences exceptional longevity (EL), i.e., reaching 100+ years of age, is more controversial.…”

Section: Introductionmentioning

confidence: 99%

ApoE gene and exceptional longevity: Insights from three independent cohorts

Garatachea

Emanuele

Calero

et al. 2014

Experimental Gerontology

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This article appeared in a journal published by Elsevier. The attached copy is furnished to the author for internal non-commercial research and education use, including for instruction at the authors institution and sharing with colleagues.Other uses, including reproduction and distribution, or selling or licensing copies, or posting to personal, institutional or third party websites are prohibited. The ApoE gene is associated with the risk of Alzheimer or cardiovascular disease but its influence on exceptional longevity (EL) is uncertain. Our primary purpose was to determine, using a case-control design, if the ApoE gene is associated with EL. We compared ApoE allele/genotype frequencies among the following cohorts: cases (centenarians, most with 1 + major disease condition; n = 163, 100-111 years) and healthy controls (n = 1039, 20-85 years) from Spain; disease-free cases (centenarians; n = 79, 100-104 years) and healthy controls (n = 597, age 27-81 years) from Italy; and cases (centenarians and semi-supercentenarians, most with 1+ major disease condition; n = 729, 100-116 years) and healthy controls (n = 498, 23-59 years) from Japan. Our main findings were twofold. First, the ε4-allele was negatively associated with EL in the three cohorts, with the following odds ratio (OR) values (adjusted by sex) having been found: 0.55 (95% confidence interval (CI): 0.33, 0.94), P = 0.030 (Spain); 0.41 (95%CI: 0.18, 0.99), P = 0.05 (Italy); and 0.35 (95%CI: 0.26, 0.57), P b 0.001 (Japan). Second, although no association was found in the Spanish cohort (OR = 1.42 (95%CI: 0.89, 2.26), P = 0.145), the ε2-allele was positively associated with EL in the Italian (OR = 2.14 (95%CI: 1.18, 3.45), P = 0.01) and Japanese subjects (OR = 1.81 (95%CI: 1.25, 2.63), P = 0.002). Notwithstanding the limitations of case-control designs, our data suggest that the ApoE might be a candidate to influence EL. The ε4-allele appears to decrease the likelihood of reaching EL among individuals of different ethnic/geographic origins. An additional, novel finding of our study was that the ε2-allele might favor EL, at least in the Italian and Japanese cohorts.

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“…A poly T repeat in an intronic polymorphism (rs10524523) (intron 6) in the TOMM40 gene, which encodes an outer mitochondrial membrane translocase involved in the transport of amyloid-β and other proteins into mitochondria, has been implicated in AD [31][32][33][34][35][36][37][38][39][40][41][42][43][44], and APOE-TOMM40 genotypes have been shown to modify disease risk and age at onset of symptoms [32][33][34][35][36][37]45], although the latter assumption needs replication due to contradictory results [36,[46][47][48][49]. A fixed-effect meta-analysis approach showed that rs4420638 at the TOMM40/APOE/APOC1 gene locus is associated with longevity [50,51]. Two independent associations with cognitive decline were found among European-Americans in the 19q13.32 region (rs769449, APOE intron; and rs115881343, TOMM40 intron); rs769449 was also associated with cognitive decline among African-Americans, but rs115881343 was not [52].…”

Section: Introductionmentioning

confidence: 99%