ESPE Abstracts (2018) 89 P-P2-181

ESPE2018 Poster Presentations Fetal, Neonatal Endocrinology and Metabolism P2 (25 abstracts)

Clinical characteristics of Congenital Hyperinsulinism Caused by Dominant KCNJ11/ABCC8 Mutations

Maria Melikyan , Diliara Gubaeva , Anatoliy Tyulpakov & Maria Kareva


Endocrine Research Center, Moscow, Russian Federation


Congenital hyperinsulinism (HI) is the most common cause of hypoglycemia in children and infants. It is characterized by a dysregulation of insulin secretion from pancreatic β-cells and mostly associated with recessive inactivating mutations in the β-cell ATP-sensitive potassium (KATP) channel genes – KCNJ11 and ABCC8. Dominantly inherited mutations in these genes are usually associated with mild forms of diazoxide responsive HI. Recently monoallelic KATP genes mutations were reported to be a rare cause of severe diazoxide unresponsive diffuse forms of HI. We report clinical and genetic characteristics of the group of patients with diazoxide unresponsive diffuse form of HI caused by a single heterozygous mutation in KATP genes. A total of 187 patients with CHI were identified in Russia since 2009. 78 of them (41.7%) were found to have monoallelic or biallelic mutations in ABCC8/KCNJ11 genes in 60 and 18 cases respectively. Most of these patients (49/78, 62.8%) were diazoxide unresponsive and 41 of 78 (52.5%) underwent pancreatic surgery. Focal form of the disease was diagnosed in 28 children (35.9%), all of them were found to carry heterozygous paternal mutation. Nine children (four females) with diazoxide unresponsive diffuse HI from 6 different families were found to have a single KCNJ11 (c.G868A:p.V290M and c.C761T:p.P254L (n=2); c.G617A:p.R206H (n=1)) or ABCC8 (c.G2143A:p.V715M (n=1); c.G2470A:p.E824K (n=2); c.C4154G:p.S1385C; (n=1) c.4153_4155del:p.1385_1385del (n=2)) mutation. In 3 families mutation was on maternal site, in 1 case - on paternal site and 2 children had denovo mutations. All but one KCNJ11 gene mutation (R206H) were previously described. Diffuse form of the disease was confirmed either by 18F-DOPA PET/CT or by histology. All of the patients had a neonatal onset of hypoglycemia, 7 of 9 were born LGA. 2 patients underwent pancreatic surgery, others were controlled with Octreotide injections and/or frequent feeds. Biochemical and clinical investigations of parents were possible in 3 families and included fasting test, standard OGTT and Hb1AC measurements. No one had hypoglycemia. In 2 families mothers who carried mutations were found to have either glucose intolerance or gestational diabetes. All the mutation carriers, including probands and those who were asymptomatic, were born LGA. In our cohort dominant KATP genes mutations account for 18,3% of the children with diffuse diazoxide unresponsive CHI. The variability of clinical presentation in mutation carriers among the family is unclear. Additional studies of possible modifying genes are needed for better understating the behavior of dominantly acting mutations.

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