Opposite Clinical Phenotypes of Glucokinase Disease: Description of a Novel Activating Mutation and Contiguous Inactivating Mutations in Human Glucokinase (GCK) Gene

doi:10.1210/me.2009-0094

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Opposite Clinical Phenotypes of Glucokinase Disease: Description of a Novel Activating Mutation and Contiguous Inactivating Mutations in Human Glucokinase (GCK) Gene

Fabrizio Barbetti^*, Nadia Cobo-Vuilleumier, Carlo Dionisi-Vici, Sonia Toni, Paolo Ciampalini, Ornella Massa, Pablo Rodriguez-Bada, Carlo Colombo, Lorenzo Lenzi, María A. Garcia-Gimeno, Francisco J. Bermudez-Silva, Fernando Rodriguez de Fonseca, Patrizia Banin, Juan C. Aledo, Elena Baixeras, Pascual Sanz, and Antonio L. Cuesta-Muñoz^*

Bambino Gesù Pediatric Hospital (F.B., C.D.-V., P.C., O.M., C.C.), Istituto di Ricovero e Cura a Carattere Scientifico, Rome 00164, Italy; Department of Internal Medicine (F.B.), University of Rome Tor Vergata, Rome 00134, Italy; Laboratory of Molecular Endocrinology and Metabolism (F.B.), S Raffaele Biomedical Park Foundation, Rome 00128, Italy; Center for the Study of Pancreatic ${beta}$ -Cell Diseases (N.C.-V., P.R.-B., F.J.B.-S., F.R.d.F., J.C.A., E.B., A.L.C.-M.). Instituto Mediterráneo para el Avance de la Biotecnología y la Investigación Sanitaria Foundation and Carlos Haya Hospital, Málaga 29010, Spain; Regional Center for Juvenile Diabetes (S.T., L.L.), Meyer Pediatric Hospital, Florence 50132, Italy; Institute of Biomedicine of Valencia (CSIC) and CIBERER-ISCIII (M.A.G.-G., P.S.), Valencia 46010, Spain; Pediatric and Adolescent Unit (P.B.), S. Anna Hospital, Ferrara, Italy; and Molecular Biology and Biochemistry Department (J.C.A.). University of Málaga, Málaga 29071, Spain

^* To whom correspondence should be addressed. E-mail: mody.2{at}libero.it; fabrizio.barbetti@spr-r.it or alcm{at}fundacionimabis.org.

Glucokinase is essential for glucose-stimulated insulin releasefrom the pancreatic ${beta}$ -cell, serving as glucose sensor in humans.Inactivating or activating mutations of glucokinase lead todifferent forms of glucokinase disease, i.e. GCK-monogenic diabetesof youth, permanent neonatal diabetes (inactivating mutations),and congenital hyperinsulinism, respectively. Here we presenta novel glucokinase gene (GCK)-activating mutation (p.E442K)found in an infant with neonatal hypoglycemia (1.5 mmol/liter)and in two other family members suffering from recurrent hypoglycemicepisodes in their childhood and adult life. In contrast to thesevere clinical presentation in the index case, functional studiesshowed only a slight activation of the protein (relative activityindex of 3.3). We also report on functional studies of two inactivatingmutations of the GCK (p.E440G and p.S441W), contiguous to theactivating one, that lead to monogenic diabetes of youth. Interestingly,adult family members carrying the GCK pE440G mutation show anunusually heterogeneous and progressive diabetic phenotype,a feature not typical of GCK-monogenic diabetes of youth. Insummary, we identified a novel activating GCK mutation thatalthough being associated with severe neonatal hypoglycemiais characterized by the mildest activation of the glucokinaseenzyme of all previously reported.

Endocrinology	Endocrine Reviews	J. Clin. End. & Metab.
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