Glucolipotoxicity of the pancreatic beta cell

Poitout, Vincent; Amyot, Julie; Semache, Meriem; Zarrouki, Bader; Hagman, Derek K.; Fontés, Ghislaine

doi:10.1016/j.bbalip.2009.08.006

Cited by 326 publications

(297 citation statements)

References 148 publications

(198 reference statements)

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“…29 This is supported by observations in INS-1E cells exposed to hyperglycemia and isolated human islets. 19,[30][31][32][33][34] Such downregulation could be due to concomitant reduction in PDX1, which is involved in regulation of insulin gene transcription and expression of other important genes involved in β-cell secretory function. 16 Reduced PDX1 levels have been observed also in HIT-T15 cells, INS-1E cells and human islets treated with high glucose.…”

Section: Discussionmentioning

confidence: 99%

Cellular responses of novel human pancreatic β-cell line, 1.1B4 to hyperglycemia

Vasu

McClenaghan²,

McCluskey

et al. 2013

Islets

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Section: Discussionmentioning

confidence: 99%

Cellular responses of novel human pancreatic β-cell line, 1.1B4 to hyperglycemia

Vasu

McClenaghan²,

McCluskey

et al. 2013

Islets

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“…8,9 Similarly, lipotoxicity arising from high fat diets triggers impairments in insulin release and eventual apoptosis. 10 Despite its central importance in metabolic physiology, the β cell in general has a poor capacity to withstand stresses, a feature that is compounded by its limited numbers and low inherent replication rate. 11 From a teleological perspective, the extent to which an individual's β cells adapt to stress may distinguish those insulin resistant individuals who develop diabetes from those who do not.…”

Section: β-Cell Dysfunction In Type 2 Diabetes Mellitusmentioning

confidence: 99%

Deoxyhypusine synthase haploinsufficiency attenuates acute cytokine signaling

et al. 2011

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“…These factors favour low grade tissue inflammation and insulin resistance [10][11][12][13][14]. The ultimate cause of hyperglycaemia, however, is insufficient insulin secretion as a consequence of impaired glucoseinduced insulin secretion (GIIS), dedifferentiated beta cells or beta cell apoptosis [15][16][17][18][19][20].…”

Section: Introductionmentioning

confidence: 99%

Metabolic crosstalk between fatty pancreas and fatty liver: effects on local inflammation and insulin secretion

et al. 2017

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Aims/hypothesis Obesity-linked ectopic fat accumulation is associated with the development of type 2 diabetes. Whether pancreatic and liver steatosis impairs insulin secretion is controversial. We examined the crosstalk of human pancreatic fat cells with islets and the role of diabetogenic factors, i.e. palmitate and fetuin-A, a hepatokine released from fatty liver. Methods Human pancreatic resections were immunohistochemically stained for insulin, glucagon, somatostatin and the macrophage/monocyte marker CD68. Pancreatic adipocytes were identified by Oil Red O and adiponectin staining.Primary pancreatic pre-adipocytes and differentiated adipocytes were co-cultured with human islets isolated from organ donors and the metabolic crosstalk between fatty liver and fatty pancreas was mimicked by the addition of palmitate and fetuin-A. Insulin secretion was evaluated by ELISA and RIA. Cytokine expression and secretion were assessed by RT-PCR and multiplex assay, respectively. Subcellular distribution of proteins was examined by confocal microscopy and protein phosphorylation by western blotting. Results In human pancreatic parenchyma, highly differentiated adipocytes were detected in the proximity of islets with normal architecture and hormone distribution. Infiltration of adipocytes was associated with an increased number of CD68-positive cells within islets. In isolated primary pancreatic preadipocytes and differentiated adipocytes, palmitate and fetuin-A induced IL6, CXCL8 and CCL2 mRNA expression. Cytokine production was toll-like receptor 4 (TLR4)-dependent and further accentuated in pre-adipocytes when cocultured with islets. In islets, IL6 and CXCL8 mRNA levels were also increased by fetuin-A and palmitate. Only in macrophages within the isolated islets, palmitate and fetuin-A stimulated the production of the cytotoxic cytokine IL-1β. Palmitate, but not fetuin-A, exerted pro-apoptotic effects in islet cells. Instead, fetuin-A impaired glucose-induced insulin secretion in a TLR4-independent, but c-Jun N-terminal kinase-and Ca 2+ -dependent, manner. Conclusions/interpretation These results provide the first evidence that fetuin-A-mediated metabolic crosstalk of fatty liver with islets may contribute to obesity-linked glucose blindness of beta cells, while fatty pancreas may exacerbate local inflammation.

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Glucolipotoxicity of the pancreatic beta cell

Cited by 326 publications

References 148 publications

Cellular responses of novel human pancreatic β-cell line, 1.1B4 to hyperglycemia

Cellular responses of novel human pancreatic β-cell line, 1.1B4 to hyperglycemia

Deoxyhypusine synthase haploinsufficiency attenuates acute cytokine signaling

Metabolic crosstalk between fatty pancreas and fatty liver: effects on local inflammation and insulin secretion

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