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The structural origin of metabolic quantitative diversity

Authors :
Jun Yasuda
Shigeo Kure
Hideyasu Kiyomoto
Seizo Koshiba
Nobuo Fuse
Tomo Saito
Matsuyuki Shirota
Daisuke Saigusa
Inaho Danjoh
Soichi Ogishima
Takako Takai-Igarashi
Yoichi Suzuki
Takanori Hasegawa
Sachiko Hirano
Kaname Kojima
Naoko Minegishi
Junichi Nakata
Shinichi Kuriyama
Kengo Kinoshita
Hozumi Motohashi
Yumi Yamaguchi-Kabata
Masao Nagasaki
Masayuki Yamamoto
Atsushi Hozawa
Miyuki Sakurai
Osamu Tanabe
Fumiki Katsuoka
Junichi Sugawara
Nobuo Yaegashi
Ikuko N. Motoike
Yosuke Kawai
Source :
Scientific Reports
Publication Year :
2016
Publisher :
Nature Publishing Group, 2016.

Abstract

Relationship between structural variants of enzymes and metabolic phenotypes in human population was investigated based on the association study of metabolite quantitative traits with whole genome sequence data for 512 individuals from a population cohort. We identified five significant associations between metabolites and non-synonymous variants. Four of these non-synonymous variants are located in enzymes involved in metabolic disorders, and structural analyses of these moderate non-synonymous variants demonstrate that they are located in peripheral regions of the catalytic sites or related regulatory domains. In contrast, two individuals with larger changes of metabolite levels were also identified, and these individuals retained rare variants, which caused non-synonymous variants located near the catalytic site. These results are the first demonstrations that variant frequency, structural location, and effect for phenotype correlate with each other in human population, and imply that metabolic individuality and susceptibility for diseases may be elicited from the moderate variants and much more deleterious but rare variants.

Details

Language :
English
ISSN :
20452322
Database :
OpenAIRE
Journal :
Scientific Reports
Accession number :
edsair.doi.dedup.....fbdff0f51a055adcb384d692ab1a5cbf
Full Text :
https://doi.org/10.1038/srep31463