PLoS ONE (Jan 2019)

Fine-scale haplotype mapping of MUT, AACS, SLC6A15 and PRKCA genes indicates association with insulin resistance of metabolic syndrome and relationship with branched chain amino acid metabolism or regulation.

  • Sara Haydar,
  • Florin Grigorescu,
  • Mădălina Vintilă,
  • Yannick Cogne,
  • Corinne Lautier,
  • Yildiz Tutuncu,
  • Jean Frederic Brun,
  • Jean Marie Robine,
  • Michel Pugeat,
  • Christophe Normand,
  • Patrick Poucheret,
  • Monica Livia Gheorghiu,
  • Carmen Georgescu,
  • Corin Badiu,
  • Nicoleta Băculescu,
  • Eric Renard,
  • Dorina Ylli,
  • Stephanie Badiou,
  • Thibault Sutra,
  • Jean Paul Cristol,
  • Jacques Mercier,
  • Ramon Gomis,
  • Josep Maria Macias,
  • Serghey Litvinov,
  • Elza Khusnutdinova,
  • Catalina Poiana,
  • Renato Pasquali,
  • Davide Lauro,
  • Giorgio Sesti,
  • Sabrina Prudente,
  • Vincenzo Trischitta,
  • Agathocles Tsatsoulis,
  • Sonia Abdelhak,
  • Abdelhamid Barakat,
  • Akila Zenati,
  • Agron Ylli,
  • Ilhan Satman,
  • Timo Kanninen,
  • Yves Rinato,
  • Sasa Missoni

DOI
https://doi.org/10.1371/journal.pone.0214122
Journal volume & issue
Vol. 14, no. 3
p. e0214122

Abstract

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Branched chain amino acids (BCAA) are essential elements of the human diet, which display increased plasma levels in obesity and regained particular interest as potential biomarkers for development of diabetes. To define determinants of insulin resistance (IR) we investigated 73 genes involved in BCAA metabolism or regulation by fine-scale haplotype mapping in two European populations with metabolic syndrome. French and Romanians (n = 465) were genotyped for SNPs (Affymetrix) and enriched by imputation (BEAGLE 4.1) at 1000 genome project density. Initial association hits detected by sliding window were refined (HAPLOVIEW 3.1 and PHASE 2.1) and correlated to homeostasis model assessment (HOMAIR) index, in vivo insulin sensitivity (SI) and BCAA plasma levels (ANOVA). Four genomic regions were associated with IR located downstream of MUT, AACS, SLC6A15 and PRKCA genes (P between 9.3 and 3.7 x 10-5). Inferred haplotypes up to 13 SNPs length were associated with IR (e.g. MUT gene with P 2.0) were correlated with in vivo insulin sensitivity (1/SI) except for SLC6A15 gene. Association of these genes with BCAA levels was variable, but influential haplotypes confirmed implication of MUT from BCAA metabolism as well as a role of regulatory genes (AACS and PRKCA) and suggested potential changes in transcriptional activity. These data drive attention towards new regulatory regions involved in IR in relation with BCAA and show the ability of haplotypes in phased DNA to detect signals complimentary to SNPs, which may be useful in designing genetic markers for clinical applications in ethnic populations.