Nonsense mutation in the glucokinase gene causes early-onset non-insulin-dependent diabetes mellitus

Vionnet, Nathalie; Stoffel, Markus; Takeda, Jun; Yasuda, Kazuki; Bell, Graeme I.; Zouali, Habib; Lesage, Suzanne; Velho, Gilberto; Iris, François; Passa, P; Froguel, P; Cohen, Daniel

doi:10.1038/356721a0

Cited by 584 publications

(316 citation statements)

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“…GK is a key regulator in the hepatic control of glucose storage and disposal [6,24]. Since GK gene expression was decreased in some diabetic patients [8,9,10], increasing GK activity in the liver appeared as an attractive approach to normalize hyperglycaemia, a common feature of both Type I and Type II diabetes. Hyperglycaemia is the main factor responsible for the development of diabetes-associated retinal, renal, neurological and vascular complications [25].…”

Section: Discussionmentioning

confidence: 99%

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Improved metabolic disorders of insulin receptor-deficient mice by transgenic overexpression of glucokinase in the liver

et al. 2002

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Aims/hypothesis. Insulin receptor null mutant mice develop severe diabetes, ketoacidosis and liver steatosis and die within 1 week after birth. Since the liver plays an essential role in the control of glucose homeostasis, we examined in this work whether the metabolic disorders of insulin receptor-deficient mice could be improved upon restoration of hepatic glucose metabolism by transgenic constitutive overexpression of glucokinase selectively in the liver. Methods. We first generated transgenic mice overexpressing rat glucokinase cDNA under control of the liver-specific phenylalanine hydroxylase gene promoter. These transgenic mice were crossed with heterozygous insulin-receptor-null mutants to produce homozygous insulin-receptor-null mice overexpressing glucokinase in the liver. Results. The transgenic mice overexpressing glucokinase in the liver showed improved glucose tolerance and were mildly hypoglycaemic and hyperlipidaemic under starved conditions. The introduction of the glucokinase transgene in insulin receptor null mice did not prevent the development of glycosuria. However, ketoacidosis was delayed by more than 1 week and survival was prolonged to 10 to 16 days in 16% of the pups. In these longer surviving pups, serum glucose and triglyceride concentrations were lowered, hepatic glycogen stores were reconstituted and liver steatosis was absent as compared with the pups which had developed strong ketoacidosis and died earlier.Conclusions/interpretation. These results show that overexpression of hepatic glucokinase can compensate, in part, for the metabolic disorders developed by insulin receptor-deficient mice. This shows the importance of improving hepatic function in diabetes and must revive interest in enhancement of glucokinase activity as a therapeutic strategy for the treatment of diabetes. [Diabetologia (2002[Diabetologia ( ) 45:1292[Diabetologia ( -1297

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Section: Discussionmentioning

confidence: 99%

“…Studies focused on GK gained particular attention since the discovery that MODY-2 is associated with mutations in the GK gene resulting in reduced GK activity in both liver and beta cells [8,9]. Lower hepatic GK activity was also reported in a group of patients with Type II (non-insulin-dependent) diabetic mellitus patients [10].…”

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confidence: 99%

Improved metabolic disorders of insulin receptor-deficient mice by transgenic overexpression of glucokinase in the liver

et al. 2002

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“…Population association studies of the GK gene locus between normoglycaemic and Type 2 diabetic American Blacks [72] and Mauritian Creoles [73] have been positive. Mutations have now been recorded in some families with MODY (Type 2 diabetes subtype presenting from the second decade with an autosomal dominant mode of inheritence) [41, [74][75][76]) and in one pedigree thought to have classic Type 2 diabetes [77] but no other mutations have yet been identified in the common variety of the disease.…”

Section: Glucokinase and Candidate Genes For Type 2 Diabetesmentioning

confidence: 99%

“…In the French study a nonsense mutation in exon 7 of the GK gene was identified [GAG (Glu) to TAG (amber termination codon)] [75] together with two further missense mutations in exon 7 (Thr-228--->Met and Gly-261--+Arg) that cosegregate with diabetes [41]. In the UK study a missense mutation in exon 8 was identified (Gly-299--->Arg) [77].…”

Section: Glucokinase Gene Mutations In Type 2 Diabetesmentioning

confidence: 99%

Glucokinase and candidate genes for Type 2 (non-insulin-dependent) diabetes mellitus

Randle

1993

Diabetologia

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“…16 different nonsense and missense mutations in the glucokinase gene have been identified in affected members ofthese MODY families (6)(7)(8)(9). These mutations were shown to impair the enzymatic activity of the encoded protein (10).…”

Section: Introductionmentioning

confidence: 99%

Deletion of the donor splice site of intron 4 in the glucokinase gene causes maturity-onset diabetes of the young.

Sun¹,

Pueyo²,

Zouali³

et al. 1993

J. Clin. Invest.

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Missense and nonsense mutations in the glucokinase gene have recently been shown to result in maturity-onset diabetes of the young (MODY), a subtype of non-insulin-dependent diabetes mellitus with early age of onset. Glucokinase catalyzes the formation of glucose-6-phosphate and is involved in the regulation of insulin secretion and integration of hepatic intermediary metabolism. Nucleotide sequence analysis of exon 4 and its flanking intronic regions of the glucokinase gene, in four hyperglycemic individuals of a MODY family, revealed a deletion of 15 base pairs, which removed the t of the gt in the donor splice site of intron 4, and the following 14 base pairs. This deletion resulted in two aberrant transcripts, which were analyzed by reverse transcription of RNA from lymphoblastoid cells obtained from a diabetic patient. In one ofthe abnormal transcripts, exon 5 is missing, while in the other, the activation of a cryptic splice site leads to the removal of the last eight codons of exon 4. This intronic deletion in a donor splice site seems to cause a more severe form of glucose intolerance, compared with point mutations described in glucokinase. This might be due to a more pronounced effect on insulin secretion. (J. Clin. Invest. 1993.

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Nonsense mutation in the glucokinase gene causes early-onset non-insulin-dependent diabetes mellitus

Cited by 584 publications

References 10 publications

Improved metabolic disorders of insulin receptor-deficient mice by transgenic overexpression of glucokinase in the liver

Improved metabolic disorders of insulin receptor-deficient mice by transgenic overexpression of glucokinase in the liver

Glucokinase and candidate genes for Type 2 (non-insulin-dependent) diabetes mellitus

Deletion of the donor splice site of intron 4 in the glucokinase gene causes maturity-onset diabetes of the young.

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