Monogenic diabetes

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作者
Amélie Bonnefond
Ranjit Unnikrishnan
Alessandro Doria
Martine Vaxillaire
Rohit N. Kulkarni
Viswanathan Mohan
Vincenzo Trischitta
Philippe Froguel
机构
[1] Lille University Hospital,Inserm UMR1283, CNRS UMR8199, European Genomic Institute for Diabetes (EGID), Institut Pasteur de Lille
[2] Université de Lille,Department of Metabolism
[3] Imperial College London,Department of Diabetology, Madras Diabetes Research Foundation
[4] Indian Council of Medical Research Centre for Advanced Research on Diabetes and Dr Mohan’s Diabetes Specialities Centre,Research Division
[5] Joslin Diabetes Center,Department of Medicine
[6] Harvard Medical School,Research Unit of Diabetes and Endocrine Diseases
[7] Fondazione IRCCS Casa Sollievo Della Sofferenza,Department of Experimental Medicine
[8] Sapienza University,undefined
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摘要
Monogenic diabetes includes several clinical conditions generally characterized by early-onset diabetes, such as neonatal diabetes, maturity-onset diabetes of the young (MODY) and various diabetes-associated syndromes. However, patients with apparent type 2 diabetes mellitus may actually have monogenic diabetes. Indeed, the same monogenic diabetes gene can contribute to different forms of diabetes with early or late onset, depending on the functional impact of the variant, and the same pathogenic variant can produce variable diabetes phenotypes, even in the same family. Monogenic diabetes is mostly caused by impaired function or development of pancreatic islets, with defective insulin secretion in the absence of obesity. The most prevalent form of monogenic diabetes is MODY, which may account for 0.5–5% of patients diagnosed with non-autoimmune diabetes but is probably underdiagnosed owing to insufficient genetic testing. Most patients with neonatal diabetes or MODY have autosomal dominant diabetes. More than 40 subtypes of monogenic diabetes have been identified to date, the most prevalent being deficiencies of GCK and HNF1A. Precision medicine approaches (including specific treatments for hyperglycaemia, monitoring associated extra-pancreatic phenotypes and/or following up clinical trajectories, especially during pregnancy) are available for some forms of monogenic diabetes (including GCK- and HNF1A-diabetes) and increase patients’ quality of life. Next-generation sequencing has made genetic diagnosis affordable, enabling effective genomic medicine in monogenic diabetes.
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