A Genome-Wide Association Study of 2304 Extreme Longevity Cases Identifies Novel Longevity Variants

Author:

Bae Harold,Gurinovich Anastasia,Karagiannis Tanya T.,Song Zeyuan,Leshchyk Anastasia,Li MengzeORCID,Andersen Stacy L.,Arbeev KonstantinORCID,Yashin Anatoliy,Zmuda Joseph,An Ping,Feitosa Mary,Giuliani Cristina,Franceschi Claudio,Garagnani Paolo,Mengel-From JonasORCID,Atzmon GilORCID,Barzilai Nir,Puca AnnibaleORCID,Schork Nicholas J.,Perls Thomas T.,Sebastiani PaolaORCID

Abstract

We performed a genome-wide association study (GWAS) of human extreme longevity (EL), defined as surviving past the 99th survival percentile, by aggregating data from four centenarian studies. The combined data included 2304 EL cases and 5879 controls. The analysis identified a locus in CDKN2B-AS1 (rs6475609, p = 7.13 × 10−8) that almost reached genome-wide significance and four additional loci that were suggestively significant. Among these, a novel rare variant (rs145265196) on chromosome 11 had much higher longevity allele frequencies in cases of Ashkenazi Jewish and Southern Italian ancestry compared to cases of other European ancestries. We also correlated EL-associated SNPs with serum proteins to link our findings to potential biological mechanisms that may be related to EL and are under genetic regulation. The findings from the proteomic analyses suggested that longevity-promoting alleles of significant genetic variants either provided EL cases with more youthful molecular profiles compared to controls or provided some form of protection from other illnesses, such as Alzheimer’s disease, and disease progressions.

Funder

NIA

Publisher

MDPI AG

Subject

Inorganic Chemistry,Organic Chemistry,Physical and Theoretical Chemistry,Computer Science Applications,Spectroscopy,Molecular Biology,General Medicine,Catalysis

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