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

Sun, Fang; Pueyo, María E.; Zouali, Habib; Lesage, Suzanne; Vaxillaire, Martine; Passa, P; Cohen, Daniel; Antignac, Corinne

doi:10.1172/jci116687

Cited by 26 publications

(13 citation statements)

References 34 publications

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“…Overwhelming evidence indicates that glucokinase is the primary component of the ␤-cell glucose-sensor apparatus and accounts for the characteristic glucose concentration dependence of insulin secretion (27,42,52). This is supported by the fact that genetic mutations in glucokinase can cause a form of type II diabetes mellitus designated maturity-onset diabetes of the young (MODY) and that catalytic activities of mutant glucokinases encoded by MODY genes are reduced (53)(54)(55). MODY is an autosomal dominant disorder and occurs despite the presence of one normal glucokinase allele (53).…”

Section: Discussionmentioning

confidence: 99%

Interleukin-1 Reduces the Glycolytic Utilization of Glucose by Pancreatic Islets and Reduces Glucokinase mRNA Content and Protein Synthesis by a Nitric Oxide-dependent Mechanism

Landt

Bohrer

et al. 1997

Journal of Biological Chemistry

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Culture of rat pancreatic islets with interleukin-1 (IL-1) results in up-regulation of the inducible isoform of nitric oxide synthase and overproduction of nitric oxide (NO). This is associated with reversible inhibition of both glucose-induced insulin secretion and islet glucose oxidation, and these effects are prevented by the inducible nitric oxide synthase inhibitor N G -monomethylarginine. IL-1 also induces accumulation of nonesterified arachidonic acid in islets by an NO-dependent mechanism, and one potential explanation for that effect would involve an IL-1-induced enhancement of islet glycolytic flux. We have therefore examined effects of IL-1 on islet glycolytic utilization of glucose and find that culture of islets with IL-1 in medium containing 5.5 mM glucose results in suppression of islet glucose utilization subsequently measured at glucose concentrations between 6 and 18 mM. The IL-1-induced suppression of islet glucose utilization is associated with a decline in islet glucokinase mRNA content, as determined by competitive reverse transcriptase-polymerase chain reaction, and in glucokinase protein synthesis, as determined by immuoprecipitation experiments, and all of these effects are prevented by N G -monomethylarginine. These findings suggest that IL-1 can down-regulate islet glucokinase, which is the primary component of the islet glucose-sensor apparatus, by an NO-dependent mechanism. Because reductions in islet glucokinase levels are known to cause a form of type II diabetes mellitus, these observations raise the possibility that factors which increase islet NO levels might contribute to development of glucose intolerance.Culture of rat pancreatic islets with interleukin-1 (IL-1)

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Section: Discussionmentioning

confidence: 99%

Interleukin-1 Reduces the Glycolytic Utilization of Glucose by Pancreatic Islets and Reduces Glucokinase mRNA Content and Protein Synthesis by a Nitric Oxide-dependent Mechanism

Landt

Bohrer

et al. 1997

Journal of Biological Chemistry

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“…Genetic investigations in families with strong diabetes aggregation have demonstrated that mutations in the coding regions of the glucokinase gene (GCK) on chromosome 7 result in a familial subtype of NIDDM, characterized by an early age of onset and autosomal dominant inheritance with high penetrance (maturity onset diabetes of young 2 [MODY 2]) (1)(2)(3)(4)(5)(6). Glucokinase phosphorylates glucose to glucose-6-phosphate and plays a major role in the regulation and integration of glucose metabolism in pancreatic ␤ cells and hepatocytes (7,8).…”

Section: Introductionmentioning

confidence: 99%

“…All GCK mutations associated with hyperglycemia that have so far been identified have been localized to exons that are common to both the pancreatic and hepatic isoforms of the enzyme (1)(2)(3)(4)(5)(6). It is therefore certain that the hepatocytes also express the mutant enzyme, although the consequences of these mutations on the hepatic metabolism of glucose, and their role in the pathogenesis of hyperglycemia remain unknown.…”

Section: Introductionmentioning

confidence: 99%

Impaired hepatic glycogen synthesis in glucokinase-deficient (MODY-2) subjects.

Velho

Petersen²,

Perseghin³

et al. 1996

J. Clin. Invest.

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201

127

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All glucokinase gene mutations identified to date have been localized to exons that are common to the pancreatic and hepatic isoforms of the enzyme. While impaired insulin secretion has been observed in glucokinase-deficient subjects the consequences of this mutation on hepatic glucose metabolism remain unknown. To examine this question hepatic glycogen concentration was measured in seven glucokinasedeficient subjects with normal glycosylated hemoglobin and 12 control subjects using 13 C nuclear magnetic spectroscopy during a day in which three isocaloric mixed meals were ingested. The relative fluxes of the direct and indirect pathways of hepatic glycogen synthesis were also assessed using [1-13 C]glucose in combination with acetaminophen to noninvasively sample the hepatic UDP-glucose pool. Average fasting hepatic glycogen content was similar in glucokinasedeficient and control subjects (279 Ϯ 20 vs 284 Ϯ 14 mM; mean Ϯ SEM), and increased in both groups after the meals with a continuous pattern throughout the day. However, the net increment in hepatic glycogen content after each meal was 30-60% lower in glucokinase-deficient than in the control subjects (breakfast, 46% lower, P Ͻ 0.02; lunch, 62% lower, P ϭ 0.002; dinner; 30% lower, P ϭ 0.04). The net increment over basal values 4 h after dinner was 105 Ϯ 18 mM in glucokinase-deficient and 148 Ϯ 11 mM in control subjects ( P ϭ 0.04). In the 4 h after breakfast, flux through the gluconeogenic pathway relative to the direct pathway of hepatic glycogen synthesis was higher in glucokinase-deficient than in control subjects (50 Ϯ 2% vs 34 Ϯ 5%; P ϭ 0.038). In conclusion glucokinase-deficient subjects have decreased net accumulation of hepatic glycogen and relatively augmented hepatic gluconeogenesis after meals. These results suggest that in addition to the altered ␤ cell function, abnormalities in liver glycogen metabolism play an important role in the pathogenesis of hyperglycemia in patients with glucokinase-deficient maturity onset diabetes of young. ( J. Clin. Invest. 1996. 98:1755-1761.)

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“…We have recently reported an assay that used the presence of ectopic transcripts within lymphoblastoid cells to examine the effect of three splice site mutations of the HNF-1α gene [18]. This approach has also been used to examine the effects of a splice site mutation in the glucokinase (GCK) gene [19].…”

Section: Introductionmentioning

confidence: 99%

Abnormal splicing of hepatocyte nuclear factor-1 beta in the renal cysts and diabetes syndrome

et al. 2004

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Aims/hypothesis. Mutations in the hepatocyte nuclear factor-1 beta (HNF-1β) gene result in disorders of renal development, typically involving renal cysts and early-onset diabetes (the RCAD syndrome/ MODY5). Sixteen mutations have been reported, including three splicing mutations of the intron 2 splice donor site. Because tissues showing abundant expression (kidney, liver, pancreas, gut, lung and gonads) are not easily accessible for analysis in living subjects, it has previously proven difficult to determine the effect of HNF-1β mutations at the mRNA level. This is the aim of the present study. Methods. We have developed a nested RT-PCR assay that exploits the presence of ectopic HNF-1β transcripts in Epstein-Barr virus (EBV)-transformed lymphoblastoid cell lines derived from subjects carrying HNF-1β splice site mutations.Results. We report a fourth mutation of the intron 2 splice donor site, IVS2nt+2insT. Sequence analysis of ectopic HNF-1β transcripts showed that both IVS2nt+2insT and IVS2nt+1G>T result in the deletion of exon 2 and are predicted to result in premature termination of the HNF-1β protein. Mutant transcripts were less abundant than the normal transcripts but there was no evidence of nonsense-mediated decay. Conclusions/interpretation. This is the first study to define the pathogenic consequences of mutations within the HNF-1β gene by mRNA analysis. This type of approach is a useful and important tool to define mutational mechanisms and determine pathogenicity.Keywords HNF-1β · Illegitimate transcription · MODY5 · RCAD · RT-PCR · Splicing. Abbreviations: Ct, crossing point · EBV, Epstein-Barr virus · HNF-1β, hepatocyte nuclear factor beta · MODY5, maturity-onset diabetes of the young subtype 5 · NMD, nonsense-mediated decay · RCAD, renal cysts and diabetes syndrome Diabetologia (2004) 47:937-942

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

Cited by 26 publications

References 34 publications

Interleukin-1 Reduces the Glycolytic Utilization of Glucose by Pancreatic Islets and Reduces Glucokinase mRNA Content and Protein Synthesis by a Nitric Oxide-dependent Mechanism

Interleukin-1 Reduces the Glycolytic Utilization of Glucose by Pancreatic Islets and Reduces Glucokinase mRNA Content and Protein Synthesis by a Nitric Oxide-dependent Mechanism

Impaired hepatic glycogen synthesis in glucokinase-deficient (MODY-2) subjects.

Abnormal splicing of hepatocyte nuclear factor-1 beta in the renal cysts and diabetes syndrome

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