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An Amish founder population reveals rare-population genetic determinants of the human lipidome. | LitMetric

AI Article Synopsis

  • The study investigates genetic factors influencing lipid species linked to cardiovascular disease (CVD) using data from the Amish founder population, which may reveal insights beyond traditional lipid measures.
  • Researchers conducted a genome-wide scan of 355 lipid species in 650 Amish individuals, discovering associations with rare lipid variants unique to this population for the first time.
  • The findings highlight the potential of studying founder populations to uncover novel genetic variants associated with lipid traits, emphasizing the importance of both rare and common variants in understanding lipidomics in relation to CVD risk.

Article Abstract

Identifying the genetic determinants of inter-individual variation in lipid species (lipidome) may provide deeper understanding and additional insight into the mechanistic effect of complex lipidomic pathways in CVD risk and progression beyond simple traditional lipids. Previous studies have been largely population based and thus only powered to discover associations with common genetic variants. Founder populations represent a powerful resource to accelerate discovery of previously unknown biology associated with rare population alleles that have risen to higher frequency due to genetic drift. We performed a genome-wide association scan of 355 lipid species in 650 individuals from the Amish founder population including 127 lipid species not previously tested. To the best of our knowledge, we report for the first time the lipid species associated with two rare-population but Amish-enriched lipid variants: APOB_rs5742904 and APOC3_rs76353203. We also identified novel associations for 3 rare-population Amish-enriched loci with several sphingolipids and with proposed potential functional/causal variant in each locus including GLTPD2_rs536055318, CERS5_rs771033566, and AKNA_rs531892793. We replicated 7 previously known common loci including novel associations with two sterols: androstenediol with UGT locus and estriol with SLC22A8/A24 locus. Our results show the double power of founder populations and detailed lipidome to discover novel trait-associated variants.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8989972PMC
http://dx.doi.org/10.1038/s42003-022-03291-2DOI Listing

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