Phthalates Rapidly Increase Production of Reactive Oxygen Species in Vivo: Role of Kupffer Cells

Introduction. Paracetamol is an effective analgesic/antipyretic drug when used at therapeutic doses. However, the overdose of paracetamol can cause severe liver injury and liver necrosis. The mechanism of paracetamol-induced liver injury is still not completely understood. Reactive metabolite formation, depletion of glutathione and alkylation of proteins are the triggers of inhibition of mitochondrial respiration, adenosine triphosphate depletion and mitochondrial oxidant stress leading to hepatocellular necrosis. Role of oxidative stress in paracetamol-induced liver injury. The importance of oxidative stress in paracetamol hepatotoxicity is controversial. Paracetamol induced liver injury cause the formation of reactive oxygen species. The potent sources of reactive oxygen are mitochondria, neutrophils, Kupffer cells and the enzyme xatnine oxidase. Free radicals lead to lipid peroxidation, enzymatic inactivation and protein oxidation. Role of mitochondria in paracetamol-induced oxidative stress. The production of mitochondrial reactive oxygen species is increased, and the glutathione content is decreased in paracetamol overdose. Oxidative stress in mitochondria leads to mito?chondrial dysfunction with adenosine triphosphate depletion, increase mitochondrial permeability transition, deoxyribonu?cleic acid fragmentation which contribute to the development of hepatocellular necrosis in the liver after paracetamol overdose. Role of Kupffer cells in paracetamol-induced liver injury. Paracetamol activates Kupffer cells, which then release numerous cytokines and signalling molecules, including nitric oxide and superoxide. Kupffer cells are important in peroxynitrite formation. On the other hand, the activated Kupffer cells release anti-inflammatory cytokines. Role of neutrophils in paracetamol-induced liver injury. Paracetamol-induced liver injury leads to the accumulation of neutrophils, which release lysosomal enzymes and generate superoxide anion radicals through the enzyme nicotinamide adenine dinucleotide phosphate oxidase. Hydrogen peroxide, which is influenced by the neutrophil-derived enzyme myeloperoxidase, generates hypochlorus acid as a potent oxidant. Role of peroxynitrite in paracetamol-induced oxidative stress. Superoxide can react with nitric oxide to form peroxynitrite, as a potent oxidant. Nitrotyrosine is formed by the reaction of tyrosine with peroxynitrite in paracetamol hepatotoxicity. Conclusion. Overdose of paracetamol may produce severe liver injury with hepatocellular necrosis. The most important mechanisms of cell injury are metabolic activation of paracetamol, glutathione depletion, alkylation of proteins, especially mitochondrial proteins, and formation of reactive oxygen/nitrogen species.

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The role of oxidative stress in alcoholic liver injury

Medicinski pregled ◽

10.2298/mpns0912547r ◽

2009 ◽

Vol 62 (11-12) ◽

pp. 547-553 ◽

Cited By ~ 22

Author(s):

Tatjana Radosavljevic ◽

Dusan Mladenovic ◽

Danijela Vucevic

Keyword(s):

Oxidative Stress ◽

Nitric Oxide ◽

Reactive Oxygen Species ◽

Liver Injury ◽

Kupffer Cells ◽

Reactive Oxygen ◽

Oxygen Species ◽

Alcoholic Liver Injury ◽

Chronic Ethanol Consumption

Introduction. Oxidative stress plays an important role in pathogenesis of alcoholic liver injury. The main source of free oxygen species is cytochrome P450-dependent monooxygenase, which can be induced by ethanol. Role of cytochrome P4502E1 in ethanol-induced oxidative stress. Reactive oxygen species produced by this enzyme are more important in intracellular oxidative damage compared to species derived from activated phagocytes. Free radicals lead to lipid peroxidation, enzymatic inactivation and protein oxidation. Role of mitochondria in alcohol-induced oxidative stress. Production of mitochondrial reactive oxygen species is increased, and glutathione content is decreased in chronically ethanolfed animals. Oxidative stress in mitochondria leads to mitochondrial DNA damage and has a dual effect on apoptosis. Role of Kupffer cells in alcohol-induced liver injury. Chronic ethanol consumption is associated with increased release of endotoxin from gut lumen into portal circulation. Endotoxin activates Kupffer cells, which then release proinflammatory cytokines and oxidants. Role of neutrophils in alcohol-induced liver injury. Alcoholic liver injury leads to the accumulation of neutrophils, which release reactive oxygen species and lysosomal enzymes and contribute to hepatocyte damage and necrosis. Role of nitric oxide in alcohol-induced oxidative stress. High amounts of nitric oxide contribute to the oxidative damage, mainly by generating peroxynitrites. Role of antioxidants in ethanol-induced oxidative stress. Chronic ethanol consumption is associated with reduced liver glutathione and ?-tocopherol level and with reduced superoxide dismutase, catalase and glutathione peroxidase activity. Conclusion. Oxidative stress in alcoholic liver disease is a consequence of increased production of oxidants and decreased antioxidant defense in the liver.

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The Role of Reactive Oxygen Species in the Light-Induced Deformation of DNA

Zeitschrift für Naturforschung B ◽

10.1515/znb-1984-0922 ◽

1984 ◽

Vol 39 (9) ◽

pp. 1276-1280 ◽

Cited By ~ 1

Author(s):

R. Baumann ◽

M. Herrmann ◽

H. Parlar

Keyword(s):

Reactive Oxygen Species ◽

Excited States ◽

Reactive Oxygen ◽

Oxygen Species ◽

In Vivo Experiments ◽

Pyrimidine Bases ◽

Effect Of Oxygen

Dimerizations and reactions with water of pyrimidine bases are the primary steps held responsible for the deformation of DNA at short wavelengths in vitro and in vivo experiments. However the influence of oxygen in combination with water on the UV deformation at wavelengths representative for troposphere is evident from the observed data and both together are needed to change the DNA structure. The only plausible explanation for the effect of oxygen is the formation of reactive oxygen species during the UV irradiation of DNA. In the present work the deformation of DNA by different oxygen species like singlet oxygen (1O2), superoxideanion (O2-), hydroxyradical (·OH), ozone (O3) and hydrogenperoxide (H2O2) is excluded with the help of chemical-trapping experiments. The photo-induced transformation proceeds via excited states of DNA. which react with groundstate oxygen to afford peroxide.

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The Role of Kupffer Cells and Reactive Oxygen Species in Hepatic Injury During Acute and Chronic Alcohol Intoxication

Alcoholism Clinical and Experimental Research ◽

10.1111/j.1530-0277.1998.tb04013.x ◽

1998 ◽

Vol 22 (s5) ◽

pp. 255S-259S ◽

Cited By ~ 20

Author(s):

Abraham P. Bautista

Keyword(s):

Reactive Oxygen Species ◽

Kupffer Cells ◽

Hepatic Injury ◽

Alcohol Intoxication ◽

Reactive Oxygen ◽

Oxygen Species ◽

Chronic Alcohol ◽

Chronic Alcohol Intoxication

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Nitrate tolerance does not increase production of peroxynitrite in the heart

AJP Heart and Circulatory Physiology ◽

10.1152/ajpheart.00817.2001 ◽

2002 ◽

Vol 283 (1) ◽

pp. H69-H76 ◽

Cited By ~ 19

Author(s):

Tamás Csont ◽

Csaba Csonka ◽

Annamária Ónody ◽

Anikó Görbe ◽

László Dux ◽

...

Keyword(s):

Reactive Oxygen Species ◽

Vascular Dysfunction ◽

Reactive Oxygen ◽

Nitrate Tolerance ◽

Oxygen Species ◽

Mechanical Function ◽

Nitrate Treatment

Clinical studies have suggested that long-term nitrate treatment does not improve and may even worsen cardiovascular mortality, and the possible role of nitrate tolerance has been suspected. Nitrate tolerance has been recently shown to increase vascular superoxide and peroxynitrite production leading to vascular dysfunction. Nevertheless, nitrates exert direct cardiac effects independent from their vascular actions. Therefore, we investigated whether in vivo nitroglycerin treatment leading to vascular nitrate tolerance increases cardiac formation of nitric oxide (NO), reactive oxygen species, and peroxynitrite, thereby leading to cardiac dysfunction. Nitrate tolerance increased bioavailability of NO in the heart without increasing formation of reactive oxygen species. Despite elevated myocardial NO, neither cardiac markers of peroxynitrite formation nor cardiac mechanical function were affected by nitroglycerin treatment. However, serum free nitrotyrosine, a marker for systemic peroxynitrite formation, was significantly elevated in nitroglycerin-treated animals. This is the first demonstration that, although the systemic effects of nitroglycerin may be deleterious due to enhancement of extracardiac peroxynitrite formation, nitroglycerin does not result in oxidative damage in the heart.

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Angiotensin II induces p27Kip1 expression in renal tubules in vivo: role of reactive oxygen species

Journal of Molecular Medicine ◽

10.1007/s001090100241 ◽

2001 ◽

Vol 79 (7) ◽

pp. 382-389 ◽

Cited By ~ 27

Author(s):

Gunter Wolf ◽

Ulrich Wenzel ◽

Tete Hannken ◽

Rolf A. Stahl

Keyword(s):

Reactive Oxygen Species ◽

Angiotensin Ii ◽

Reactive Oxygen ◽

Renal Tubules ◽

Oxygen Species ◽

P27kip1 Expression

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Attenuation of Ischemia-Induced Mouse Brain Injury by SAG, a Redox-Inducible Antioxidant Protein

Journal of Cerebral Blood Flow & Metabolism ◽

10.1097/00004647-200106000-00010 ◽

2001 ◽

Vol 21 (6) ◽

pp. 722-733 ◽

Cited By ~ 44

Author(s):

Guo-Yuan Yang ◽

Li Pang ◽

Hai-Liang Ge ◽

Mingjia Tan ◽

Wen Ye ◽

...

Keyword(s):

Reactive Oxygen Species ◽

Brain Injury ◽

Mouse Brain ◽

Ischemia Reperfusion ◽

Reactive Oxygen ◽

Model Systems ◽

Oxygen Species ◽

Antioxidant Protein

Cerebral ischemia resulting from a disruption of blood flow to the brain initiates a cascade of events that causes neuron death and leads to neurologic dysfunction. Reactive oxygen species are thought, at least in part, to mediate this disease process. The authors recently cloned and characterized an antioxidant protein, SAG (sensitive to apoptosis gene), that is redox inducible and protects cells from apoptosis induced by redox agents in a number of in vitro cell model systems. This study reports a neuroprotective role of SAG in ischemia/reperfusion-induced brain injury in an in vivo mouse model. SAG was expressed at a low level in brain tissue and was inducible after middle cerebral artery occlusion with peak expression at 6 to 12 hours. At the cellular level, SAG was mainly expressed in the cytoplasm of neurons and astrocytes, revealed by double immunofluorescence. An injection of recombinant adenoviral vector carrying human SAG into mouse brain produced an overexpression of SAG protein in the injected areas. Transduction of AdCMVSAG (wild-type), but not AdCMVmSAG (mutant), nor the AdCMVlacZ control, protected brain cells from ischemic brain injury, as evidenced by significant reduction of the infarct areas where SAG was highly expressed. The result suggests a rather specific protective role of SAG in the current in vivo model. Mechanistically, SAG overexpression decreased reactive oxygen species production and reduced the number of apoptotic cells in the ischemic areas. Thus, antioxidant SAG appears to protect against reactive oxygen species–induced brain damage in mice. Identification of SAG as a neuroprotective molecule could lead to potential stroke therapies.

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