Common variant in MTNR1B associated with increased risk of type 2 diabetes and impaired early insulin secretion.

Valeriya Lyssenko, Cecilia Nagorny, Michael R Erdos, Nils Wierup, Anna Jonsson, Peter Spégel, Marco Bugliani, Richa Saxena, Malin Fex, Nicolo Pulizzi, Bo Isomaa, Tiinamaija Tuomi, Peter Nilsson, Johanna Kuusisto, Jaakko Tuomilehto, Michael Boehnke, David Altshuler, Frank Sundler, Johan G Eriksson, Anne U JacksonMarkku Laakso, Piero Marchetti, Richard M Watanabe, Hindrik Mulder, Leif Groop

Research output: Contribution to journalArticlepeer-review

Abstract

Genome-wide association studies have shown that variation in MTNR1B (melatonin receptor 1B) is associated with insulin and glucose concentrations. Here we show that the risk genotype of this SNP predicts future type 2 diabetes (T2D) in two large prospective studies. Specifically, the risk genotype was associated with impairment of early insulin response to both oral and intravenous glucose and with faster deterioration of insulin secretion over time. We also show that the MTNR1B mRNA is expressed in human islets, and immunocytochemistry confirms that it is primarily localized in beta cells in islets. Nondiabetic individuals carrying the risk allele and individuals with T2D showed increased expression of the receptor in islets. Insulin release from clonal beta cells in response to glucose was inhibited in the presence of melatonin. These data suggest that the circulating hormone melatonin, which is predominantly released from the pineal gland in the brain, is involved in the pathogenesis of T2D. Given the increased expression of MTNR1B in individuals at risk of T2D, the pathogenic effects are likely exerted via a direct inhibitory effect on beta cells. In view of these results, blocking the melatonin ligand-receptor system could be a therapeutic avenue in T2D.
Original languageEnglish
Pages (from-to)82-88
JournalNature Genetics
Volume41
Issue number1
DOIs
Publication statusPublished - 2009

Bibliographical note

The information about affiliations in this record was updated in December 2015.
The record was previously connected to the following departments: Diabetes and Endocrinology (013241530), Internal Medicine Research Unit (013242520), Diabetes and Celiac Unit (013241540), Endocrinology (013241500), Neuroendocrine Cell Biology (013212008), Molecular Metabolism (013212001)

Subject classification (UKÄ)

  • Endocrinology and Diabetes

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