Macrosomia and Hyperinsulinaemic Hypoglycaemia in Patients with Heterozygous Mutations in the HNF4A Gene
Top Cited Papers
Open Access
- 3 April 2007
- journal article
- research article
- Published by Public Library of Science (PLoS) in PLoS Medicine
- Vol. 4 (4) , e118
- https://doi.org/10.1371/journal.pmed.0040118
Abstract
Macrosomia is associated with considerable neonatal and maternal morbidity. Factors that predict macrosomia are poorly understood. The increased rate of macrosomia in the offspring of pregnant women with diabetes and in congenital hyperinsulinaemia is mediated by increased foetal insulin secretion. We assessed the in utero and neonatal role of two key regulators of pancreatic insulin secretion by studying birthweight and the incidence of neonatal hypoglycaemia in patients with heterozygous mutations in the maturity-onset diabetes of the young (MODY) genes HNF4A (encoding HNF-4α) and HNF1A/TCF1 (encoding HNF-1α), and the effect of pancreatic deletion of Hnf4a on foetal and neonatal insulin secretion in mice. We examined birthweight and hypoglycaemia in 108 patients from families with diabetes due to HNF4A mutations, and 134 patients from families with HNF1A mutations. Birthweight was increased by a median of 790 g in HNF4A-mutation carriers compared to non-mutation family members (p < 0.001); 56% (30/54) of HNF4A-mutation carriers were macrosomic compared with 13% (7/54) of non-mutation family members (p < 0.001). Transient hypoglycaemia was reported in 8/54 infants with heterozygous HNF4A mutations, but was reported in none of 54 non-mutation carriers (p = 0.003). There was documented hyperinsulinaemia in three cases. Birthweight and prevalence of neonatal hypoglycaemia were not increased in HNF1A-mutation carriers. Mice with pancreatic β-cell deletion of Hnf4a had hyperinsulinaemia in utero and hyperinsulinaemic hypoglycaemia at birth. HNF4A mutations are associated with a considerable increase in birthweight and macrosomia, and are a novel cause of neonatal hypoglycaemia. This study establishes a key role for HNF4A in determining foetal birthweight, and uncovers an unanticipated feature of the natural history of HNF4A-deficient diabetes, with hyperinsulinaemia at birth evolving to decreased insulin secretion and diabetes later in life.Keywords
This publication has 39 references indexed in Scilit:
- Activating Mutations in theABCC8Gene in Neonatal Diabetes MellitusNew England Journal of Medicine, 2006
- A Conditional Model Reveals That Induction of Hepatocyte Nuclear Factor-1α inHnf1α-Null Mutant β-Cells Can Activate Silenced Genes Postnatally, Whereas Overexpression Is DeleteriousDiabetes, 2006
- A heterozygous activating mutation in the sulphonylurea receptor SUR1 (ABCC8) causes neonatal diabetesHuman Molecular Genetics, 2006
- Activating Mutations in the Gene Encoding the ATP-Sensitive Potassium-Channel Subunit Kir6.2 and Permanent Neonatal DiabetesNew England Journal of Medicine, 2004
- Dominantly inherited hyperinsulinism caused by a mutation in the sulfonylurea receptor type 1Journal of Clinical Investigation, 2000
- Familial Hyperinsulinism Caused by an Activating Glucokinase MutationNew England Journal of Medicine, 1998
- Familial Persistent Hyperinsulinemic Hypoglycemia of Infancy and Mutations in the Sulfonylurea ReceptorNew England Journal of Medicine, 1997
- Mutation of the pancreatic islet inward rectifier Kir6.2 also leads to familial persistent hyperinsulinemic hypoglycemia of infancyHuman Molecular Genetics, 1996
- Early neonatal death in mice homozygous for a null allele of the insulin receptor geneNature Genetics, 1996
- Cross sectional stature and weight reference curves for the UK, 1990.Archives of Disease in Childhood, 1995