G6PC2: A Negative Regulator of Basal Glucose-Stimulated Insulin Secretion

Pound, Lynley D.; Oeser, James K.; O’Brien, Tracy P.; Wang, Yingda; Faulman, Chandler J.; Dadi, Prasanna K.; Jacobson, David A.; Hutton, John C.; McGuinness, Owen P.; Shiota, Masakazu; O’Brien, Richard M.

doi:10.2337/db12-1067

Cited by 70 publications

(141 citation statements)

References 42 publications

(75 reference statements)

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“…GSE72719) (Ingenuity Pathway Analysis presented in Supplementary Table 4). Interestingly, G6pc2, one of the most highly expressed genes in β-cells (9), was strongly repressed in islets from SRI-tg10 mice. Subsequent qRT-PCR analysis in isolated islets from SRI-tg10, SRI-tg1, and Sri −/− mice confirmed the inverse relationship between Sri and G6pc2 expression levels (Fig.…”

Section: Resultsmentioning

confidence: 99%

Sorcin Links Pancreatic β-Cell Lipotoxicity to ER Ca2+ Stores

et al. 2016

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Preserving β-cell function during the development of obesity and insulin resistance would limit the worldwide epidemic of type 2 diabetes. Endoplasmic reticulum (ER) calcium (Ca2+) depletion induced by saturated free fatty acids and cytokines causes β-cell ER stress and apoptosis, but the molecular mechanisms behind these phenomena are still poorly understood. Here, we demonstrate that palmitate-induced sorcin downregulation and subsequent increases in glucose-6-phosphatase catalytic subunit-2 (G6PC2) levels contribute to lipotoxicity. Sorcin is a calcium sensor protein involved in maintaining ER Ca2+ by inhibiting ryanodine receptor activity and playing a role in terminating Ca2+-induced Ca2+ release. G6PC2, a genome-wide association study gene associated with fasting blood glucose, is a negative regulator of glucose-stimulated insulin secretion (GSIS). High-fat feeding in mice and chronic exposure of human islets to palmitate decreases endogenous sorcin expression while levels of G6PC2 mRNA increase. Sorcin-null mice are glucose intolerant, with markedly impaired GSIS and increased expression of G6pc2. Under high-fat diet, mice overexpressing sorcin in the β-cell display improved glucose tolerance, fasting blood glucose, and GSIS, whereas G6PC2 levels are decreased and cytosolic and ER Ca2+ are increased in transgenic islets. Sorcin may thus provide a target for intervention in type 2 diabetes.

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Section: Resultsmentioning

confidence: 99%

Sorcin Links Pancreatic β-Cell Lipotoxicity to ER Ca2+ Stores

et al. 2016

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“…In contrast, key metabolic genes that are either considered 'disallowed' or contribute to their regulation (Dhawan et al, 2015;MartinezSanchez et al, 2016;Piccand et al, 2014;Pullen and Rutter, 2013) were enriched in immature beta cells ( Figure 3E). Islets were also co-stained for insulin, Ucn3, and 8 G6pc2, which hydrolyzes glucose-6-phosphate (Pound et al, 2013) or the oxidoreductase Ero1lb, which is required for disulfide bond formation in pro-insulin (Zito et al, 2010). Both markers co-labeled Ucn3-positive mature beta cells, and the majority of Ucn3 negative beta cells did not express G6pc2 or Ero1lb ( Figure 3F-I).…”

Section: Ucn3 Negative Beta Cells Are Transcriptionally Immaturementioning

confidence: 99%

Virgin Beta Cells Persist throughout Life at a Neogenic Niche within Pancreatic Islets

et al. 2017

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“…This variant has in previous studies been found to be associated with elevated fasting glucose [15] and it likely regulates the expression of G6PC2 encoding the catalytic subunit of glucose-6-phosphatase, a regulator of glycolytic flux in the beta cell. The major allele is proposed to cause a rightward shift of the dose-response curve for the glucosestimulated insulin secretion [16], which explains the association with HOMA-B and insulinogenic index in opposite directions.…”

Section: Discussionmentioning

confidence: 99%

Genetic and phenotypic correlations between surrogate measures of insulin release obtained from OGTT data

et al. 2015

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Aims/hypothesis We examined the extent to which surrogate measures of insulin release have shared genetic causes. Methods Genetic and phenotypic correlations were calculated in a family cohort (n=315) in which beta cell indices were estimated based on fasting and oral glucose-stimulated plasma glucose, serum C-peptide and serum insulin levels. Furthermore, we genotyped a large population-based cohort (n= 6,269) for common genetic variants known to associate with type 2 diabetes, fasting plasma glucose levels or fasting serum insulin levels to examine their association with various indices. Results We found a notable difference between the phenotypic and genetic correlations for the traits, emphasising that the phenotypic correlation is an insufficient measure of the magnitude of shared genetic impact. In addition, we found that corrected insulin response, insulinogenic index and incAUC for insulin after an oral glucose challenge shared the majority of their genetic backgrounds, with genetic correlations of 0.80-0.99. The BIGTT index for acute insulin response differed slightly more from the latter with genetic correlations of 0.78-0.87. The HOMA for beta cell function was genetically closely related to fasting insulin with a genetic correlation of 0.85. The effects of 82 selected susceptibility single nucleotide polymorphisms on these insulin secretion indices supported our interpretation of the data and added insight into the biological differences between the examined traits. Conclusions/interpretation The level of shared genetic background varies between surrogate measures of insulin release, and this should be considered when designing a genetic association study to best obtain information on various mechanisms of insulin release.

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G6PC2: A Negative Regulator of Basal Glucose-Stimulated Insulin Secretion

Cited by 70 publications

References 42 publications

Sorcin Links Pancreatic β-Cell Lipotoxicity to ER Ca2+ Stores

Sorcin Links Pancreatic β-Cell Lipotoxicity to ER Ca2+ Stores

Virgin Beta Cells Persist throughout Life at a Neogenic Niche within Pancreatic Islets

Genetic and phenotypic correlations between surrogate measures of insulin release obtained from OGTT data

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