Prostaglandin E2 Mediates Inhibition of Insulin Secretion by Interleukin-1β

Tran, Phuong Oanh T.; Gleason, Catherine E.; Poitout, Vincent; Robertson, R. Paul

doi:10.1074/jbc.274.44.31245

Cited by 94 publications

(114 citation statements)

References 29 publications

(45 reference statements)

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“…Increases in islet IL-1␤ during the development of diabetes in an animal model have been reported (7). We reported that specific inhibitors of cyclooxygenase-2 and PGE 2 production prevent IL-1␤ from inhibiting glucose-induced insulin secretion in isolated islets (14). However, the effect of IL-1␤ that inhibits insulin secretion via ROS formation we identified in the current study appears to be independent from PGE 2 production because PGE 2 did not increase ROS levels.…”

Section: Discussioncontrasting

confidence: 54%

“…However, the effect of IL-1␤ that inhibits insulin secretion via ROS formation we identified in the current study appears to be independent from PGE 2 production because PGE 2 did not increase ROS levels. The effect of IL-1␤ that is mediated by PGE 2 to inhibit glucoseinduced insulin secretion may be more potent than the corresponding ROS-mediated effect of IL-1␤ because GCLC overexpression only partially prevented the IL-1␤ inhibitory effect on insulin secretion, whereas treatment with specific cyclooxygenase-2 inhibitors completely prevented IL-1␤-induced inhibition of glucose-induced insulin secretion (14).…”

Section: Discussionmentioning

confidence: 99%

“…Sciences and an ABI Prism 7700 Sequence detector equipped with a thermocycler (Taqman TM technology) and a cooled charge-coupled device camera to detect fluorescence emission over a range of wavelengths (500 -650 nm) as described previously by our laboratory (14). Probe and primers designed to detect GCLC expression levels were based on the sequence for rat GCLC (GenBank TM accession number AF218362 (17)) and were designed to target the same region as probes used for Northern blot analyses as reported previously in the literature (18,19).…”

Section: Methodsmentioning

confidence: 99%

“…Isolation and Culture of Wistar Rat Islets-Islets from the pancreata of male Wistar rats were isolated and cultured as described previously (6,14).…”

Section: Methodsmentioning

confidence: 99%

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Adenoviral Overexpression of the Glutamylcysteine Ligase Catalytic Subunit Protects Pancreatic Islets against Oxidative Stress

Tran

Parker

Leroy

et al. 2004

Journal of Biological Chemistry

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The catalytic subunit of glutamylcysteine ligase (GCLC) primarily regulates de novo synthesis of glutathione (GSH) in mammalian cells and is central to the antioxidant capacity of the cell. However, GCLC expression in pancreatic islets has not been previously examined. We designed experiments to ascertain whether GCLC is normally expressed in islets and whether it is up-regulated by interleukin-1␤ (IL-1␤). GCLC expression levels were intermediate compared with other metabolic tissues (kidney, liver, muscle, fat, and lung). IL-1␤ up-regulated GCLC expression (10 ng/ml IL-1␤, 3.76 ؎ 0.86; 100 ng/ml IL-1␤, 4.22 ؎ 0.68-fold control) via the p38 form of mitogen-activated protein kinase and NF B and also increased reactive oxygen species levels (10 ng/ml IL-1␤, 5.41 ؎ 1.8-fold control). This was accompanied by an increase in intraislet GSH/GSSG ratio (control, 7.1 ؎ 0.1; 10 ng/ml IL-1␤, 8.0 ؎ 0.5; 100 ng/ml IL-1␤, 8.2 ؎ 0.5-fold control; p < 0.05). To determine whether overexpression of GCLC increases the antioxidant capacity of the islet and prevents the adverse effects of IL-1␤ on glucose-induced insulin secretion, islets were infected with an adenovirus encoding GCLC. IL-1␤ significantly decreased glucose-stimulated insulin secretion (control, 123.8 ؎ 17.7; IL-1␤, 40.2 ؎ 3.9 microunits/ml insulin/islet). GCLC overexpression increased intraislet GSH levels and partially prevented the decrease in glucose-stimulated insulin secretion caused by IL-1␤. These data provide the first report of GCLC expression in the islet and demonstrate that adenoviral overexpression of GCLC increases intracellular GSH levels and protects the beta cell from the adverse effects of IL-1␤.Glutamylcysteine ligase (GCL) 1 is the primary and ratelimiting enzyme responsible for de novo synthesis of intracellular glutathione (GSH). This enzyme catalyzes ATP-dependent ligation of L-glutamate and L-cysteine to form ␥-glutamyl-L-cysteine, which undergoes another ATP-dependent ligation with glycine catalyzed by glutathione synthetase to form the final GSH product (1, 2). GCL is a heterodimer, composed of a light regulatory subunit as well as a heavy catalytic subunit. Although both are required for optimal enzyme activity, overexpression of the catalytic subunit GCLC alone is sufficient to increase enzyme activity significantly over control levels (1). The regulation of GCL expression and activity has been studied in many other cell types, including mesangial and endothelial cells, but not the pancreatic islet. Long term exposure to high glucose levels decreases GCL expression in mesangial, retinal Muller, and endothelial cells, which results in a decrease in GSH levels (3-5). Long term exposure to high glucose conditions inhibits endothelial cells from responding to cytokine exposure with an increase in GCL expression and activity (3). That the pathogenesis of diabetes mellitus involves interactions with IL-1␤ and oxidative stress secondary to chronic hyperglycemia (6, 7) raises the questions of whether GCL is normally expressed in the islet and whe...

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Section: Discussioncontrasting

confidence: 54%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

“…Isolation and Culture of Wistar Rat Islets-Islets from the pancreata of male Wistar rats were isolated and cultured as described previously (6,14).…”

Section: Methodsmentioning

confidence: 99%

See 2 more Smart Citations

Adenoviral Overexpression of the Glutamylcysteine Ligase Catalytic Subunit Protects Pancreatic Islets against Oxidative Stress

Tran

Parker

Leroy

et al. 2004

Journal of Biological Chemistry

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“…In contrast to most mammalian cells, beta cells constitutively and dominantly produce the COX-2 isoform of PGE 2 -generating enzymes rather than COX-1 [5]. Prior studies have demonstrated that PGE 2 inhibits glucose-stimulated insulin secretion (GSIS) in clonal beta cells and isolated islets [6,7], and that selective inhibition of COX-2 attenuates the development of diabetes in the low-dose streptozotocin mouse model and protects rat islets from cytokine-induced inhibition of GSIS [8,9]. Despite the established role of PGE 2 in pancreatic beta cells, the exact molecular mechanisms of PGE 2 -mediated inhibition of insulin secretion remain poorly understood.…”

mentioning

confidence: 99%

Prostaglandin E2 regulates Foxo activity via the Akt pathway: implications for pancreatic islet beta cell dysfunction

et al. 2006

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Aims/hypothesis Prostaglandin E 2 (PGE 2 ) is a well-recognised inhibitor of glucose-stimulated insulin secretion (GSIS). The aim of this study was to investigate the signalling pathway of PGE 2 in beta cell function regulation in HIT-T15 cells and isolated rat islets. Materials and methods mRNA levels of the prostaglandin E receptor 3 (Ptger3) were measured by real-time PCR. Western blot analysis was used to detect changes in the levels of PTGER3, phosphorylated and total Akt, phosphorylated and total forkhead box 'Other' (Foxo). Transient transfection and reporter assays were used to measure Foxo transcriptional activity. The biological significance of PGE 2 in beta cell function was analysed using MTT, flow cytometry and GSIS assays. Results We found that treating HIT-T15 cells with exogenous PGE 2 stimulated Ptger3 gene expression specifically, and diminished cAMP generation. These were accompanied by the downregulation of Akt and Foxo phosphorylation in HIT-T15 cells and isolated rat islets. Moreover, PGE 2 upregulated basal and partially reversed constitutively active Akt-inactivated Foxo transcriptional activity. Furthermore, GSIS was impaired in PGE 2 -treated HIT-T15 cells and isolated islets. However, the dosage used in the above experiments did not affect beta cell viability and apoptosis. In addition, insulin-like growth factor 1 (IGF-1) pretreatment reversed the effects of PGE 2 , and wortmannin treatment abolished the preventive effects of IGF-1. Conclusions/interpretation Our observations strongly suggest that PGE 2 can induce pancreatic beta cell dysfunction through the induction of Ptger3 gene expression and inhibition of Akt/Foxo phosphorylation without impacting beta cell viability. These results shed light on the mechanisms of PGE 2 actions in pancreatic beta cell dysfunction.

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Prostaglandin E synthase 2 (PTGES2) Arg298His polymorphism and parameters of the metabolic syndrome

Lindner

Helwig

Rubin

et al. 2007

Molecular Nutrition Food Res

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The prostaglandin E synthase 2 (PTGES2) gene maps to a locus linked to obesity and is involved in the synthesis of the antilipolytic compound prostaglandin E(2). In a recent study, we found an association of the minor PTGES2 Arg298His allele and lower risk of type 2 diabetes mellitus in the European Investigation into Cancer and Nutrition (EPIC) and Cooperative Health Research in the Augsburg Region (KORA) cohorts. Here, we employed our Metabolic Intervention Cohort Kiel (MICK) to assess the influence of the PTGES2 Arg298His polymorphism on a wider scale of parameters of the metabolic syndrome and postprandial metabolism. In comparison to subjects homozygous for the Arg allele, carriers of the His-allele showed significantly lower fasting insulin (geometric mean +/- SEM: 11.8 muU/mL, 11.41-12.25 versus 13.0, 12.71-13.33; p = 0.023), lower postprandial insulin levels after an oral glucose tolerance test (area under the curve 77.2, 74.07-80.52 versus 81.2, 78.8-83.63; p = 0.023) and lower homeostasis model assessment (HOMA)-insulin-resistance (3.030, 2.909-3.157 versus 3.346, 3.257-3.438; p = 0.041) and HOMA-beta-cell-function (107.2, 104.04-110.52 versus 117.2, 114.65-119.71; p = 0.019). Adjustment for body mass index (BMI) resulted in a loss of these significant differences. BMI tended to show lower values in His-allele carriers, (p = 0.067). In conclusion, risk-reducing effects of the minor His allele of the PTGES2 Arg298His polymorphism could be mediated partly by lowered BMI.

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Prostaglandin E2 Mediates Inhibition of Insulin Secretion by Interleukin-1β

Cited by 94 publications

References 29 publications

Adenoviral Overexpression of the Glutamylcysteine Ligase Catalytic Subunit Protects Pancreatic Islets against Oxidative Stress

Adenoviral Overexpression of the Glutamylcysteine Ligase Catalytic Subunit Protects Pancreatic Islets against Oxidative Stress

Prostaglandin E2 regulates Foxo activity via the Akt pathway: implications for pancreatic islet beta cell dysfunction

Prostaglandin E synthase 2 (PTGES2) Arg298His polymorphism and parameters of the metabolic syndrome

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