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Whole-Genome Sequencing Analysis of Human Metabolome in Multi-Ethnic Populations.

Elena Valeryevna FeofanovaMichael R BrownTaryn AlkisAstrid M ManuelXihao LiUsman A TahirZilin LiKevin M MendezRachel S KellyQibin QiHan ChenMartin G LarsonRozenn N LemaitreAlanna C MorrisonCharles GrieserKari E WongRobert E GersztenZhong-Ming ZhaoJessica Lasky-Sunull nullBing Yu
Published in: Nature communications (2023)
Circulating metabolite levels may reflect the state of the human organism in health and disease, however, the genetic architecture of metabolites is not fully understood. We have performed a whole-genome sequencing association analysis of both common and rare variants in up to 11,840 multi-ethnic participants from five studies with up to 1666 circulating metabolites. We have discovered 1985 novel variant-metabolite associations, and validated 761 locus-metabolite associations reported previously. Seventy-nine novel variant-metabolite associations have been replicated, including three genetic loci located on the X chromosome that have demonstrated its involvement in metabolic regulation. Gene-based analysis have provided further support for seven metabolite-replicated loci pairs and their biologically plausible genes. Among those novel replicated variant-metabolite pairs, follow-up analyses have revealed that 26 metabolites have colocalized with 21 tissues, seven metabolite-disease outcome associations have been putatively causal, and 7 metabolites might be regulated by plasma protein levels. Our results have depicted the genetic contribution to circulating metabolite levels, providing additional insights into understanding human disease.
Keyphrases
  • genome wide
  • endothelial cells
  • copy number
  • ms ms
  • healthcare
  • induced pluripotent stem cells
  • public health
  • gene expression
  • genome wide association study
  • data analysis
  • genetic diversity
  • amino acid