Src activation generates reactive oxygen species and impairs metabolism–secretion coupling in diabetic Goto–Kakizaki and ouabain-treated rat pancreatic islets

Kominato, Rieko; Fujimoto, Shimpei; Mukai, Eri; Nakamura, Yasuhiko; Nabe, Koichiro; Shimodahira, Makiko; Nishi, Yuichi; Funakoshi, Shogo; Seino, Yutaka; Inagaki, Nobuya

doi:10.1007/s00125-008-1008-x

Cited by 37 publications

(39 citation statements)

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“…To clarify the link between reduced mitochondrial ATP production in the presence of substrates metabolizable in the Krebs cycle and reduced glucose oxidation by rapamycin, recovery of insulin release and ATP content in the presence of high glucose by ROS scavengers and activity of enzymes in the Krebs cycle were examined. Ouabain-induced endogenous ROS suppresses mitochondrial metabolism in the Krebs cycle, subsequently reducing ATP production, and reduces glucose-induced insulin release and ATP levels in the presence of high glucose, which is recovered by the suppression of endogenous ROS production and by ROS scavenge (Kajikawa et al 2002, Kominato et al 2008). High glucose raises ROS level in b-cells (Bindokas et al 2003, Sakai et al 2003, which is also found in our previous study (Kominato et al 2008).…”

Section: Discussionmentioning

confidence: 99%

“…Ouabain-induced endogenous ROS suppresses mitochondrial metabolism in the Krebs cycle, subsequently reducing ATP production, and reduces glucose-induced insulin release and ATP levels in the presence of high glucose, which is recovered by the suppression of endogenous ROS production and by ROS scavenge (Kajikawa et al 2002, Kominato et al 2008). High glucose raises ROS level in b-cells (Bindokas et al 2003, Sakai et al 2003, which is also found in our previous study (Kominato et al 2008). However, our previous study shows that ROS scavenging does not affect glucose-induced insulin secretion from control islets, but increases that from GK-diabetic islets.…”

Section: Discussionmentioning

confidence: 99%

“…ATP contents were determined as previously described (Kominato et al 2008). Briefly, after groups of cultured islets were preincubated at 2 .…”

Section: Measurement Of Atp Contentmentioning

confidence: 99%

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Rapamycin impairs metabolism-secretion coupling in rat pancreatic islets by suppressing carbohydrate metabolism

Shimodahira

Fujimoto

Mukai³

et al. 2009

Journal of Endocrinology

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Rapamycin, an immunosuppressant used in human transplantation, impairs b-cell function, but the mechanism is unclear. Chronic (24 h) exposure to rapamycin concentration dependently suppressed 16 . 7 mM glucose-induced insulin release from islets (1 . 65G0 . 06 2G3 . 3 pmol/islet per 90 min, control, nZ9, P!0 . 01). Immunoblotting revealed that the expression of complex I, III, IV, and V was not affected by rapamycin. Mitochondrial ATP production indicated that the respiratory chain downstream of complex II was not affected, but that carbohydrate metabolism in the Krebs cycle was reduced by rapamycin. Analysis of enzymes in the Krebs cycle revealed that activity of a-ketoglutarate dehydrogenase (KGDH), which catalyzes one of the slowest reactions in the Krebs cycle, was reduced by rapamycin (10 . 08G0 . 82, rapamycin versus 13 . 82 G0 . 84 nmol/mg mitochondrial protein per min, control, nZ5, P!0 . 01). Considered together, these findings indicate that rapamycin suppresses high glucose-induced insulin secretion from pancreatic islets by reducing mitochondrial ATP production through suppression of carbohydrate metabolism in the Krebs cycle, together with reduced KGDH activity.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Rapamycin impairs metabolism-secretion coupling in rat pancreatic islets by suppressing carbohydrate metabolism

Shimodahira

Fujimoto

Mukai³

et al. 2009

Journal of Endocrinology

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“…Fluorescence was determined using a spectrofluorophotometer (RF-5300PC; Shimazu, Kyoto, Japan) with excitation wavelength at 502 nm and emission wavelength at 523 nm. After 1 h incubation in the presence or absence of metformin, rotenone, ONOO − or hydrogen peroxide with or without RNS scavenger (5 mmol/l α-tocopherol plus 2.3 mmol/l ascorbate) [27], fluorescence was measured and presented as a ratio with respect to the value at time zero.…”

Section: Determination Of Reactive Nitrogen Species Onoomentioning

confidence: 99%

Metformin suppresses hepatic gluconeogenesis and lowers fasting blood glucose levels through reactive nitrogen species in mice

et al. 2010

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Aims/hypothesis Metformin, the major target of which is liver, is commonly used to treat type 2 diabetes. Although metformin activates AMP-activated protein kinase (AMPK) in hepatocytes, the mechanism of activation is still not well known. To investigate AMPK activation by metformin in liver, we examined the role of reactive nitrogen species (RNS) in suppression of hepatic gluconeogenesis. Methods To determine RNS, we performed fluorescence examination and immunocytochemical staining in mouse hepatocytes. Since metformin is a mild mitochondrial complex I inhibitor, we compared its effects on suppression of gluconeogenesis, AMPK activation and generation of the RNS peroxynitrite (ONOO − ) with those of rotenone, a representative complex I inhibitor. To determine whether endogenous nitric oxide production is required for ONOO − generation and metformin action, we used mice lacking endothelial nitric oxide synthase (eNOS). Results Metformin and rotenone significantly decreased gluconeogenesis and increased phosphorylation of AMPK in wild-type mouse hepatocytes. However, unlike rotenone, metformin did not increase the AMP/ATP ratio.

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“…Because of their fundamental importance to cell homeostasis by governing signal-transduction processes, kinases -especially members of the Rous sarcoma virus oncogene protein kinases (Src) and protein kinase C (PKC) families -are commonly crucial in various pathologies. Intriguingly, homologous to the Src and/or PKC activation was found to govern multiple pathological processes in hyperglycemia [21][22][23] and lipotoxicity [24,25]. Because similar pathways were also described as leading to cellular differentiation [17], the actual physiological outcome might depend on the pattern of activated pathways rather than on a single phenomenon.…”

Section: The Dark Side Of Mitochondrial Protein Phosphorylationmentioning

confidence: 99%

Mitochondrial protein phosphorylation: instigator or target of lipotoxicity?

Graier

Malli

Kostner

2009

Trends in Endocrinology & Metabolism

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Lipotoxicity occurs as a consequence of chronic exposure of non-adipose tissue and cells to elevated concentrations of fatty acids, triglycerides and/or cholesterol. The contribution of mitochondria to lipotoxic cell dysfunction, damage and death is associated with elevated production of reactive oxygen species and initiation of apoptosis. Although there is a broad consensus on the involvement of these phenomena with lipotoxicity, the molecular mechanisms that initiate, mediate and trigger mitochondrial dysfunction in response to substrate overload remain unclear. Here, we focus on protein phosphorylation as an important phenomenon in lipotoxicity that harms mitochondria-related signal transduction and integration in cellular metabolism. Moreover, the degradation of mitochondria by mitophagy is discussed as an important landmark that leads to cellular apoptosis in lipotoxicity. Mitochondrial relay functionThe term 'lipotoxicity' describes the dysfunction of non-adipose tissue and cells that face chronic exposure to elevated fatty acids, triglycerides and/or cholesterol [1][2][3]. When plasma levels of prandial and postprandial fatty acids, triglycerides or cholesterol exceed the uptake capacity of adipose tissue, non-adipose tissue becomes overloaded with lipids, resulting in several metabolic imbalances and/or diseases. Once the oxidative capacity of these cells is exhausted, lipotoxic pathways are initiated that yield cellular dysfunction and, at worst, result in cell death. Although multiple lipotoxic events have been described [1][2][3] (e.g. induction of endoplasmic reticulum stress [4,5] by disruption of its structural integrity [6]) recent findings point to mitochondrial dysfunction as a key phenomenon in lipotoxicity leading to ominous signals [7][8][9][10][11].The mitochondria not only serve as the power plant of the cell but also act as a cellular relay, sensing multiple cellular and environmental parameters, including energy status, oxygen availability and activation patterns of cellular signal-transduction pathways. Mitochondria then integrate these inputs, adapting their activity and functions to, ultimately, tune cellular responsiveness with respect to the current demand of the cell [12] (Figure 1). In spite of the important tasks of the mitochondrion and in contrast to its functions in energy metabolism, its contribution to signal transduction has not been thoroughly investigated, and the [24,25]. Because similar pathways were also described as leading to cellular differentiation [17], the actual physiological outcome might depend on the pattern of activated pathways rather than on a single phenomenon. Thus, it is feasible that changes in the mitochondrial phosphoproteome caused by alterations in kinase activities are fundamental for the decisive setting of signaling patterns for cell survival or the initiation of cellular dysfunction in lipotoxicity leading to cell death. Three different scenarios affecting mitochondrial protein phosphorylation can be postulated in lipotoxicity ( Figure ...

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Src activation generates reactive oxygen species and impairs metabolism–secretion coupling in diabetic Goto–Kakizaki and ouabain-treated rat pancreatic islets

Cited by 37 publications

References 49 publications

Rapamycin impairs metabolism-secretion coupling in rat pancreatic islets by suppressing carbohydrate metabolism

Rapamycin impairs metabolism-secretion coupling in rat pancreatic islets by suppressing carbohydrate metabolism

Metformin suppresses hepatic gluconeogenesis and lowers fasting blood glucose levels through reactive nitrogen species in mice

Mitochondrial protein phosphorylation: instigator or target of lipotoxicity?

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