Abstract
Thiazolidinediones are a new class of antidiabetic agent that improve insulin sensitivity and reduce plasma glucose and blood pressure in subjects with type 2 diabetes1. Although these agents can bind and activate an orphan nuclear receptor, peroxisome proliferator-activated receptor gamma (PPARγ), there is no direct evidence to conclusively implicate this receptor in the regulation of mammalian glucose homeostasis2. Here we report two different heterozygous mutations in the ligand-binding domain of PPARγ in three subjects with severe insulin resistance. In the PPARγ crystal structure, the mutations destabilize helix 12 which mediates transactivation. Consistent with this, both receptor mutants are markedly transcriptionally impaired and, moreover, are able to inhibit the action of coexpressed wild-type PPARγ in a dominant negative manner. In addition to insulin resistance, all three subjects developed type 2 diabetes mellitus and hypertension at an unusually early age. Our findings represent the first germline loss-of-function mutations in PPARγ and provide compelling genetic evidence that this receptor is important in the control of insulin sensitivity, glucose homeostasis and blood pressure in man.
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Acknowledgements
M. Gurnell is a Wellcome Training Fellow, and S. O'Rahilly and K. Chatterjee are supported by the Wellcome Trust. We thank M. Flynn, A. Marshall and J. Keogh for assistance with clinical investigations, A. Rudenski for HOMA analysis, and S. Smith (SmithKline Beecham) for PPAR γ ligands. Among the many people at Incyte Europe involved in this project, we thank C. Baynes and J. Lightning for sequencing, I. Loudon for project management support; P. Weller and E. Génin for paternity testing and analysis, and C. Luccarini and D. Townley for PPARγ genomic structure determination.
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Barroso, I., Gurnell, M., Crowley, V. et al. Dominant negative mutations in human PPARγ associated with severe insulin resistance, diabetes mellitus and hypertension. Nature 402, 880–883 (1999). https://doi.org/10.1038/47254
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DOI: https://doi.org/10.1038/47254
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