Abstract
BackgroundNeuron-derived orphan receptor (Nor) 1, nuclear receptor (Nur) 77, and nuclear receptor-related protein (Nurr) 1 constitute the NR4A family of orphan nuclear receptors which were recently found to modulate hepatic glucose production, insulin signalling in adipocytes, and oxidative metabolism in skeletal muscle. In this study, we assessed whether common genetic variation within the NR4A3 locus, encoding Nor-1, contributes to the development of prediabetic phenotypes, such as glucose intolerance, insulin resistance, or β-cell dysfunction.MethodsWe genotyped 1495 non-diabetic subjects from Southern Germany for the five tagging single nucleotide polymorphisms (SNPs) rs7047636, rs1526267, rs2416879, rs12686676, and rs10819699 (minor allele frequencies ≥ 0.05) covering 100% of genetic variation within the NR4A3 locus (with D' = 1.0, r2 ≥ 0.9) and assessed their association with metabolic data derived from the fasting state, an oral glucose tolerance test (OGTT), and a hyperinsulinemic-euglycemic clamp (subgroup, N = 506). SNPs that revealed consistent associations with prediabetic phenotypes were subsequently genotyped in a second cohort (METSIM Study; Finland; N = 5265) for replication.ResultsAll five SNPs were in Hardy-Weinberg equilibrium (p ≥ 0.7, all). The minor alleles of three SNPs, i.e., rs1526267, rs12686676, and rs10819699, consistently tended to associate with higher insulin release as derived from plasma insulin at 30 min(OGTT), AUCC-peptide-to-AUCGluc ratio and the AUCIns30-to-AUCGluc30 ratio with rs12686676 reaching the level of significance (p ≤ 0.03, all; additive model). The association of the SNP rs12686676 with insulin secretion was replicated in the METSIM cohort (p ≤ 0.03, additive model). There was no consistent association with glucose tolerance or insulin resistance in both study cohorts.ConclusionWe conclude that common genetic variation within the NR4A3 locus determines insulin secretion. Thus, NR4A3 represents a novel candidate gene for β-cell function which was not covered by the SNP arrays of recent genome-wide association studies for type 2 diabetes mellitus.
Highlights
Neuron-derived orphan receptor (Nor) 1, nuclear receptor (Nur) 77, and nuclear receptor-related protein (Nurr) 1 constitute the NR4A family of orphan nuclear receptors which were recently found to modulate hepatic glucose production, insulin signalling in adipocytes, and oxidative metabolism in skeletal muscle
We genotyped 1495 non-diabetic subjects from Southern Germany for the five tagging single nucleotide polymorphisms (SNPs) rs7047636, rs1526267, rs2416879, rs12686676, and rs10819699 (minor allele frequencies (MAFs) ≥ 0.05) covering 100% of genetic variation within the NR4A3 locus and assessed their association with metabolic data derived from the fasting state, an oral glucose tolerance test (OGTT), and, in a subgroup of 506 subjects, from a hyperinsulinemic-euglycemic clamp
Study population The TÜF/TULIP Study cohort of 1495 (506 male/989 female) non-diabetic subjects had a mean age of 39 ± 13 years. 10% had an impaired fasting glucose (IFG), 9.5% showed an impaired glucose tolerance (IGT) and 7.6% presented with both IFG and IGT in the OGTT
Summary
Neuron-derived orphan receptor (Nor) 1, nuclear receptor (Nur) 77, and nuclear receptor-related protein (Nurr) 1 constitute the NR4A family of orphan nuclear receptors which were recently found to modulate hepatic glucose production, insulin signalling in adipocytes, and oxidative metabolism in skeletal muscle. The NR4A family of orphan nuclear receptors comprises nuclear receptor (Nur) 77 (gene: NR4A1), nuclear receptor-related protein (Nurr) 1 (gene: NR4A2), and neuronderived orphan receptor (Nor) 1 (gene: NR4A3) These ligand-independent constitutively active transcription factors are co-expressed in many metabolically relevant tissues, such as skeletal muscle, adipose tissue, liver, heart, and brain, and are thought to be predominantly regulated at the transcriptional level (for review, see [1]). In 3T3-L1 adipocytes, NR4A1 (Nur-77) and NR4A3 (Nor-1) expression was reported to be induced upon insulin and thiazolidinedione treatment
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