Mutants of glucokinase cause hypoglycaemia- and hyperglycaemia syndromes and their analysis illuminates fundamental quantitative concepts of glucose homeostasis

Mutants of glucokinase cause hypoglycaemia- and hyperglycaemia syndromes and their analysis illuminates fundamental quantitative concepts of glucose homeostasis

Mutations of the glucokinase gene cause hyperglycaemia or hypoglycaemia. A quantitative understanding of these defects of glucose homeostasis linked to the glucokinase gene was lacking. Therefore a database of kinetic variables of wild-type and 20 missense mutants of glucokinase was developed and us...

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Veröffentlicht in:Diabetologia 1999-10, Vol.42 (10), p.1175-1186
Hauptverfasser: DAVIS, E. A, CUESTA-MUNOZ, A, RAOUL, M, BUETTGER, C, SWEET, I, MOATES, M, MAGNUSON, M. A, MATSCHINSKY, F. M
Format: Artikel
Sprache:eng
Schlagworte:
Adaptor Proteins, Signal Transducing
Adenosine Triphosphate - metabolism
Biological and medical sciences
Biophysics
Blood Glucose - metabolism
Carrier Proteins
Diabetes
Endocrine pancreas
Enzyme Activation - drug effects
Enzyme Activation - genetics
Enzyme Stability
Fundamental and applied biological sciences. Psychology
Glucokinase - antagonists & inhibitors
Glucokinase - genetics
Glucokinase - metabolism
Glucose
Glucose - pharmacology
Glucose - physiology
Glutathione Transferase - genetics
Homeostasis
Hormones. Régulation
Humans
Hyperglycemia
Hyperglycemia - blood
Hyperglycemia - genetics
Hypoglycemia
Hypoglycemia - blood
Hypoglycemia - genetics
Insulin
Insulin - blood
Kinetics
Mathematical models
Models, Biological
Mutation
Phosphorylation
Physiology
Proteins
Proteins - pharmacology
Recombinant Fusion Proteins - genetics
Recombinant Fusion Proteins - isolation & purification
Recombinant Fusion Proteins - metabolism
Sensors
Syndrome
Vertebrates: endocrinology
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Zusammenfassung:Mutations of the glucokinase gene cause hyperglycaemia or hypoglycaemia. A quantitative understanding of these defects of glucose homeostasis linked to the glucokinase gene was lacking. Therefore a database of kinetic variables of wild-type and 20 missense mutants of glucokinase was developed and used in mathematical modelling to predict the thresholds for glucose-stimulated insulin release. Recombinant human glucokinase was generated in E. coli. The k(cat), glucose S(0.5), ATP K(m), and Hill number of glucokinase were determined. Inhibition by Stearoyl CoA and glucokinase regulatory protein and thermal stability were assayed for all mutants kinetically similar to wild-type glucokinase. A mathematical model predicting the threshold for glucose-stimulated insulin release was constructed. This model is based on the two substrate kinetics of glucokinase and the kinetic variables of the database. It is assumed that both glucokinase gene alleles are equally expressed in beta-cells and that induction of glucokinase occurs as a function of basal blood glucose. Large changes, varying greatly between mutants were found in nearly all variables. Glucokinase flux at threshold for glucose-stimulated insulin release was about 25 % of total phosphorylating potential in the normal beta-cell and this was used to predict thresholds for the mutant heterozygotes. Clinical data for maturity onset diabetes of the young type linked to the glucokinase gene and familial hyperinsulinaemic hypoglycaemia linked to the glucokinase gene and the glucokinase kinetic data of this study were used to test the model. The model predicts fasting blood glucose between 3 and 7 mmol/l in these cases. A kinetics database of wild-type and 20 mutants of glucokinase was developed. Many kinetic differences were found for the mutants. The mathematical model to calculate the threshold for glucose-stimulated insulin release predicts fasting blood glucose between 3 and 7 mmol/l in subjects with glucokinase gene mutations. [Diabetologia 42: 1175-1186]
ISSN:0012-186X
1432-0428
DOI:10.1007/s001250051289