Animal model for maturity-onset diabetes of the young generated by disruption of the mouse glucokinase gene

D. Bali; A. Svetlanov; H. W. Lee; D. Fusco-DeMane; M. Leiser; B. Li; N. Barzilai; M. Surana; H. Hou; N. Fleischer; R. DePinho; L. Rossetti; S. Efrat

doi:10.1074/jbc.270.37.21464

Animal model for maturity-onset diabetes of the young generated by disruption of the mouse glucokinase gene

D. Bali, A. Svetlanov, H. W. Lee, D. Fusco-DeMane, M. Leiser, B. Li, N. Barzilai, M. Surana, H. Hou, N. Fleischer, R. DePinho, L. Rossetti, S. Efrat

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Abstract

Glucokinase catalyzes a rate-limiting step in glucose metabolism in hepatocytes and pancreatic β cells and is considered the 'glucose sensor' for regulation of insulin secretion. Patients with maturity-onset diabetes of the young (MODY) have heterozygous point mutations in the glucokinase gene that result in reduced enzymatic activity and decreased insulin secretion. However, it remains unclear whether abnormal liver glucose metabolism contributes to the MODY disease. Here we show that disruption of the glucokinase gene results in a phenotype similar to MODY in heterozygous mice. Reduced islet glucokinase activity causes mildly elevated fasting blood glucose levels. Hyperglycemic clamp studies reveal decreased glucose tolerance and abnormal liver glucose metabolism. These findings demonstrate a key role for glucokinase in glucose homeostasis and implicate both islets and liver in the MODY disease.

Original language	English
Pages (from-to)	21464-21467
Number of pages	4
Journal	Journal of Biological Chemistry
Volume	270
Issue number	37
DOIs	https://doi.org/10.1074/jbc.270.37.21464
Publication status	Published - 1995

All Science Journal Classification (ASJC) codes

Biochemistry
Molecular Biology
Cell Biology

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Bali, D., Svetlanov, A., Lee, H. W., Fusco-DeMane, D., Leiser, M., Li, B., Barzilai, N., Surana, M., Hou, H., Fleischer, N., DePinho, R., Rossetti, L., & Efrat, S. (1995). Animal model for maturity-onset diabetes of the young generated by disruption of the mouse glucokinase gene. Journal of Biological Chemistry, 270(37), 21464-21467. https://doi.org/10.1074/jbc.270.37.21464

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abstract = "Glucokinase catalyzes a rate-limiting step in glucose metabolism in hepatocytes and pancreatic β cells and is considered the 'glucose sensor' for regulation of insulin secretion. Patients with maturity-onset diabetes of the young (MODY) have heterozygous point mutations in the glucokinase gene that result in reduced enzymatic activity and decreased insulin secretion. However, it remains unclear whether abnormal liver glucose metabolism contributes to the MODY disease. Here we show that disruption of the glucokinase gene results in a phenotype similar to MODY in heterozygous mice. Reduced islet glucokinase activity causes mildly elevated fasting blood glucose levels. Hyperglycemic clamp studies reveal decreased glucose tolerance and abnormal liver glucose metabolism. These findings demonstrate a key role for glucokinase in glucose homeostasis and implicate both islets and liver in the MODY disease.",

author = "D. Bali and A. Svetlanov and Lee, {H. W.} and D. Fusco-DeMane and M. Leiser and B. Li and N. Barzilai and M. Surana and H. Hou and N. Fleischer and R. DePinho and L. Rossetti and S. Efrat",

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Bali, D, Svetlanov, A, Lee, HW, Fusco-DeMane, D, Leiser, M, Li, B, Barzilai, N, Surana, M, Hou, H, Fleischer, N, DePinho, R, Rossetti, L & Efrat, S 1995, 'Animal model for maturity-onset diabetes of the young generated by disruption of the mouse glucokinase gene', Journal of Biological Chemistry, vol. 270, no. 37, pp. 21464-21467. https://doi.org/10.1074/jbc.270.37.21464

TY - JOUR

T1 - Animal model for maturity-onset diabetes of the young generated by disruption of the mouse glucokinase gene

AU - Bali, D.

AU - Svetlanov, A.

AU - Lee, H. W.

AU - Fusco-DeMane, D.

AU - Leiser, M.

AU - Li, B.

AU - Barzilai, N.

AU - Surana, M.

AU - Hou, H.

AU - Fleischer, N.

AU - DePinho, R.

AU - Rossetti, L.

AU - Efrat, S.

PY - 1995

Y1 - 1995

N2 - Glucokinase catalyzes a rate-limiting step in glucose metabolism in hepatocytes and pancreatic β cells and is considered the 'glucose sensor' for regulation of insulin secretion. Patients with maturity-onset diabetes of the young (MODY) have heterozygous point mutations in the glucokinase gene that result in reduced enzymatic activity and decreased insulin secretion. However, it remains unclear whether abnormal liver glucose metabolism contributes to the MODY disease. Here we show that disruption of the glucokinase gene results in a phenotype similar to MODY in heterozygous mice. Reduced islet glucokinase activity causes mildly elevated fasting blood glucose levels. Hyperglycemic clamp studies reveal decreased glucose tolerance and abnormal liver glucose metabolism. These findings demonstrate a key role for glucokinase in glucose homeostasis and implicate both islets and liver in the MODY disease.

AB - Glucokinase catalyzes a rate-limiting step in glucose metabolism in hepatocytes and pancreatic β cells and is considered the 'glucose sensor' for regulation of insulin secretion. Patients with maturity-onset diabetes of the young (MODY) have heterozygous point mutations in the glucokinase gene that result in reduced enzymatic activity and decreased insulin secretion. However, it remains unclear whether abnormal liver glucose metabolism contributes to the MODY disease. Here we show that disruption of the glucokinase gene results in a phenotype similar to MODY in heterozygous mice. Reduced islet glucokinase activity causes mildly elevated fasting blood glucose levels. Hyperglycemic clamp studies reveal decreased glucose tolerance and abnormal liver glucose metabolism. These findings demonstrate a key role for glucokinase in glucose homeostasis and implicate both islets and liver in the MODY disease.

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Animal model for maturity-onset diabetes of the young generated by disruption of the mouse glucokinase gene

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