Non-esterified fatty acids are deleterious for human pancreatic islet function at physiological glucose concentration

Dubois, Mathilde; Kerr–Conte, Julie; Gmyr, Valéry; Bouckenooghe, Thomas; Muharram, Ghaffar; d’Herbomez, Michèle; Martin-Ponthieu, Annie; Vantyghem, Marie-Christine; Vandewalle, B.; Pattou, François

doi:10.1007/s00125-004-1347-1

Cited by 63 publications

(48 citation statements)

References 44 publications

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“…As previously reported in human islets (24,25), incubation with fatty acids for 48 h resulted in triglyceride accumulation (P Ͻ 0.001) and apoptosis of islets (P Ͻ 0.001) (Fig. 7D and E).…”

Section: Diabetes Vol 55 June 2006supporting

confidence: 85%

Peroxisome Proliferator–Activated Receptor α Improves Pancreatic Adaptation to Insulin Resistance in Obese Mice and Reduces Lipotoxicity in Human Islets

et al. 2006

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Peroxisome proliferator-activated receptor (PPAR) ␣ is a transcription factor controlling lipid and glucose homeostasis. PPAR␣-deficient (؊/؊) mice are protected from high-fat diet-induced insulin resistance. However, the impact of PPAR␣ in the pathophysiological setting of obesityrelated insulin resistance is unknown. Therefore, PPAR␣ ؊/؊ mice in an obese (ob/ob) background were generated. PPAR␣ deficiency did not influence the growth curves of the obese mice but surprisingly resulted in a severe, age-dependent hyperglycemia. PPAR␣ deficiency did not aggravate peripheral insulin resistance. By contrast, PPAR␣ ؊/؊ ob/ob mice developed pancreatic ␤-cell dysfunction characterized by reduced mean islet area and decreased insulin secretion in response to glucose in vitro and in vivo. In primary human pancreatic islets, PPAR␣ agonist treatment prevented fatty acid-induced impairment of glucose-stimulated insulin secretion, apoptosis, and triglyceride accumulation. These results indicate that PPAR␣ improves the adaptative response of the pancreatic ␤-cell to pathological conditions. PPAR␣ could thus represent a promising target in the prevention of type 2 diabetes.

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Section: Diabetes Vol 55 June 2006supporting

confidence: 85%

Peroxisome Proliferator–Activated Receptor α Improves Pancreatic Adaptation to Insulin Resistance in Obese Mice and Reduces Lipotoxicity in Human Islets

et al. 2006

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“…Preparation of islets, cell culture, secretion assays, immunofluorescence, determination of cAMP and CREactivation Rat islets or human donor islets were obtained and cultured as described [18,19] and approved by the ethics committee. For calcium imaging, rat islet cells were seeded on polylysine-coated glass coverslips (6,000/coverslip, 25 mm diameter) and precultured for 4 days at 11 mmol/l glucose before transfection with lipofectamine.…”

Section: Methodsmentioning

confidence: 99%

Adenylyl cyclase 8 is central to glucagon-like peptide 1 signalling and effects of chronically elevated glucose in rat and human pancreatic beta cells

et al. 2010

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Aims/hypothesis Glucose and incretins regulate beta cell function, gene expression and insulin exocytosis via calcium and cAMP. Prolonged exposure to elevated glucose (also termed glucotoxicity) disturbs calcium homeostasis, but little is known about cAMP signalling. We therefore investigated long-term effects of glucose on this pathway with special regard to the incretin glucagon-like peptide 1 (GLP-1). Methods We exposed INS-1E cells and rat or human islets to different levels of glucose for 3 days and determined functional responses in terms of second messengers (cAMP, Ca 2+ ), transcription profiles, activation of cAMP-responsive element (CRE) and secretion by measuring membrane capacitance. Moreover, we modulated directly the abundance of a calcium-sensitive adenylyl cyclase (ADCY8) and GLP-1 receptor (GLP1R).Results GLP-1-or forskolin-mediated increases in cytosolic calcium, cAMP-levels or insulin secretion were largely reduced in INS-1E cells cultured at elevated glucose (>5.5 mmol/l). Statistical analysis of transcription profiles identified cAMP pathways as major targets regulated by glucose. Quantitative PCR confirmed these findings and unravelled marked downregulation of the calcium-sensitive adenylyl cyclase ADCY8 also in rat and in human islets. Re-expression of ADCY8, but not of the GLP1R, recovered GLP-1 signalling in glucotoxicity in INS-1E cells and in rat islets. Moreover, knockdown of this adenylyl cyclase showed that GLP-1-induced cAMP generation, calcium signalling, activation of the downstream target CRE and direct amplification of exocytosis by cAMP-raising agents (evaluated by capacitance measurement) proceeds via ADCY8. Conclusions/interpretation cAMP-mediated pathways are modelled by glucose, and downregulation of the calcium-B. Roger and J. Papin contributed equally to this study. Electronic supplementary material The online version of this article

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“…Exposure of rat islets to elevated plasma NEFA concentration, which has long-term (inhibitory) and short-term (stimulatory) effects on glucose-stimulated insulin secretion, did increase UCP2 abundance (Lameloise et al 2001). This contrasts with our negative association between mean plasma NEFA and pancreatic UCP2 following leptin administration, suggesting a decrease in UCP2 may allow the pancreatic -cells to resist the detrimental effects of high NEFA exposure (Dubois et al 2004, Joseph et al 2004. Increased NEFA metabolism leads to an increase in energy flux through the electron transport chain, which can lead to enhanced production of reactive oxygen species in -cells (Carlsson et al 1999, Barbu et al 2002.…”

Section: Leptin and Ucp2 In The Neonatal Pancreasmentioning

confidence: 58%

Tissue-specific effects of leptin administration on the abundance of mitochondrial proteins during neonatal development

Gnanalingham¹,

Mostyn²,

Wang³

et al. 2005

Journal of Endocrinology

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Many tissues undergo a rapid transition after birth, accompanied by dramatic changes in mitochondrial protein function. In particular, uncoupling protein (UCP) abundance increases at birth in the lung and adipose tissue, to then gradually decline, an adaptation that is important in enabling normal tissue function. Leptin potentially mediates some of these changes and is known to promote the loss of UCP1 from brown fat but its effects on UCP2 and related mitochondrial proteins (i.e. voltage-dependent anion channel (VDAC) and cytochrome c) in other tissues are unknown. We therefore determined the effects of once-daily jugular venous administration of ovine recombinant leptin on mitochondrial protein abundance as determined by immunoblotting in tissues that do (i.e. the brain and pancreas) and do not (i.e. liver and skeletal muscle) express UCP2. Eight pairs of 1-day-old lambs received either 100 µg leptin or vehicle daily for 6 days, before tissue sampling on day 7. Administration of leptin diminished UCP2 abundance in the pancreas, but not the brain. Leptin administration had no affect on the abundance of VDAC or cytochrome c in any tissue examined. In leptin-administered animals, but not controls, UCP2 abundance in the pancreas was positively correlated with VDAC and cytochrome c content, and UCP2 abundance in the brain with colonic temperature. In conclusion, leptin administration to neonatal lambs causes a tissuespecific loss of UCP2 from the pancreas. These effects may be important in the regulation of neonatal tissue development and potentially for optimising metabolic control mechanisms in later life.

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Non-esterified fatty acids are deleterious for human pancreatic islet function at physiological glucose concentration

Cited by 63 publications

References 44 publications

Peroxisome Proliferator–Activated Receptor α Improves Pancreatic Adaptation to Insulin Resistance in Obese Mice and Reduces Lipotoxicity in Human Islets

Peroxisome Proliferator–Activated Receptor α Improves Pancreatic Adaptation to Insulin Resistance in Obese Mice and Reduces Lipotoxicity in Human Islets

Adenylyl cyclase 8 is central to glucagon-like peptide 1 signalling and effects of chronically elevated glucose in rat and human pancreatic beta cells

Tissue-specific effects of leptin administration on the abundance of mitochondrial proteins during neonatal development

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