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            -Arginine Treatment Alters the Kinetics of Nitric Oxide and Superoxide Release and Reduces Ischemia/Reperfusion Injury in Skeletal Muscle

Huk, I.; Nanobashvili, J.; Neumayer, Christoph; Punz, A.; Mueller, M; Afkhampour, Kaweh; Mittlböck, Martina; Losert, Udo; Polterauer, P; Roth, Erich; Patton, Stephen R.; Maliński, Tadeusz

doi:10.1161/01.cir.96.2.667

Cited by 221 publications

(190 citation statements)

References 26 publications

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“…Recently, evidence has accumulated that O 2 Ϫ production and its interaction with NO, yielding the strong oxidant ONOO Ϫ , play central roles in vascular pathophysiology. 6 The present study demonstrates race-specific differences in endothelial NO bioavailability and ONOO Ϫ formation. These differences arise because endothelial cells from blacks generate significantly more O 2 Ϫ , primarily from 2 enzymatic sources: NAD(P)H-oxidase and eNOS.…”

Section: Discussionsupporting

confidence: 52%

“…Compared with whites, the steady state of NO/O 2 Ϫ /ONOO Ϫ balance in the endo- thelial cells from blacks is kept closer to the redox state that had been documented in the endothelium-impaired function disorders. 3,6,15,23 …”

Section: Discussionmentioning

confidence: 99%

“…In the majority of cases, the source of O 2 Ϫ excess is uncertain, although involvement of NAD(P)H-dependent oxidases, xanthine oxidase, cyclooxygenase, mitochondrial oxidases, and endothelial nitric oxide synthase (eNOS) and neuronal NOS have been suggested. [3][4][5][6] It should be noted that the net effect of the reaction between NO and O 2 Ϫ compromises reduction of concentration of both substrates as well as biological effects of ONOO Ϫ itself. Peroxynitrite induces the oxidation of proteins, DNA, and lipids in vascular walls.…”

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confidence: 99%

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Race-Specific Differences in Endothelial Function

2004

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Background-The prevalence of the endothelium-impaired function disorders, such as hypertension and diabetes mellitus, and the severity of their complications are considerably greater in blacks than whites. Evidence has accumulated that superoxide (O 2 Ϫ ) production and its interaction with nitric oxide (NO), yielding the strong oxidant peroxynitrite (ONOO Ϫ ), play central roles in vascular pathophysiology. We hypothesized that the differences in endothelial NO/O 2 Ϫ /ONOO Ϫ metabolism may highlight the potential predisposition to endothelial dysfunction and cardiovascular complications prevalent in blacks. Methods and Results-Highly sensitive tandem electrochemical NO/O 2 Ϫ /ONOO Ϫ nanosensors were positioned in single human umbilical vein endothelial cells (HUVECs) isolated from blacks and whites, and the kinetics of NO/O 2 Ϫ /ONOO

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Section: Discussionsupporting

confidence: 52%

Section: Discussionmentioning

confidence: 99%

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confidence: 99%

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Race-Specific Differences in Endothelial Function

2004

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“…Loss of NOS III activity, caused by either loss or inactivation of NOS III protein, would be expected to result in vasoconstriction, neutrophil extravasation, and edema, which could contribute to cell death by extending the episode of ischemia through the "no-reflow" phenomenon (Ames et al, 1968;Kanwar and Kubes, 1995;Kubes, 1993;Menger et al 1997). Pharmacological treatments that increase NO levels early during reperfusion or ischemic pre-conditioning (which is in part NOS III-mediated), protect skeletal muscle from IRmediated constriction and edema (Akimitsu et al, 1995;Chen et al, 1998;Huk et al, 1997;Pudupakkam et al, 1998). However, there is a dissociation between early vascular reperfusion and neutrophil infiltration from parenchymal injury and death in skeletal muscle IR (Breidahl et al, 1996;Hickey et al, 1996;Skjeldal et al, 1993Skjeldal et al, , 1994.…”

Section: Messina Et Almentioning

confidence: 99%

Localization of Inducible Nitric Oxide Synthase to Mast Cells During Ischemia/Reperfusion Injury of Skeletal Muscle

Messina

Knight

Dowsing

et al. 2000

Laboratory Investigation

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SUMMARY:Nitric oxide contributes to tissue necrosis after ischemia-reperfusion (IR). A biochemical and immunohistochemical study was made of the amounts and localization of both Ca ϩϩ -independent nitric oxide synthase (NOS) II and Ca ϩϩ -dependent (NOS I and NOS III) in rat skeletal muscle after ischemia and 0.5, 2, 8, 16, and 24 hours reperfusion. NOS II was not detectable in control muscle or during ischemia, was first detected after 2 hours reperfusion, increased further by 8 hours, and remained elevated at 24 hours. Both NOS II and nitrotyrosine, a marker of peroxynitrite formation, were localized exclusively to mast cells except after 24 hours reperfusion when some macrophages and neutrophils also showed positive immunoreactivity. Mast cells underwent extensive degranulation during reperfusion. NOS I was not detected in injured or control muscle. The level of NOS III, which was localized to the endothelium of blood vessels of all sizes in control muscle, decreased progressively during ischemia and reperfusion to reach undetectable levels after 16 hours reperfusion. These findings indicate that most of the nitric oxide formed during IR injury is generated by NOS II located almost exclusively in mast cells. (Lab Invest 2000, 80:423-431).

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“…1 In addition, abnormally low NO concentrations (Ͻ1 nmol/L) have been measured in microvessels in vivo during ischemia/reperfusion (I/R) by use of porphyrinic microsensors. 2 Reestablishing blood flow to ischemic tissues or organs (reperfusion) is an essential step in many surgical procedures. 3 Especially after prolonged ischemia, however, reperfusion can lead to changes in vasomotility and an increase in microvascular permeability causing tissue reperfusion edema.…”

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S -Nitroso Human Serum Albumin Treatment Reduces Ischemia/Reperfusion Injury in Skeletal Muscle via Nitric Oxide Release

et al. 2002

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Background-Peroxynitrite generated from nitric oxide (NO) and superoxide (O 2 Ϫ ) contributes to ischemia/reperfusion (I/R) injury. Feedback inhibition of endothelial NO synthase by NO may inhibit O 2 Ϫ production generated also by endothelial NO synthase at diminished local L-arginine concentrations accompanying I/R. Methods and Results-During hindlimb I/R (2.5 hours/2 hours), in vivo NO was monitored continuously (porphyrinic sensor), and high-energy phosphates, reduced and oxidized glutathione (chromatography), and I/R injury were measured intermittently. Rabbits receiving human serum albumin (HSA) (controls) were compared with those receiving S-nitroso human serum albumin (S-NO-HSA) beginning 30 minutes before reperfusion for 1 hour or 30 minutes before ischemia for 3.5 hours (0.1 mol · kg Ϫ1 · h Ϫ1 ). The onset of ischemia led to a rapid increase of NO from its basal level (50Ϯ12 nmol/L) to 120Ϯ20 and 220Ϯ15 nmol/L in the control and S-NO-HSA-treated groups, respectively. In control animals, NO dropped below basal levels at the end of ischemia and to undetectable levels (Ͻ1 nmol/L) during reperfusion. In S-NO-HSA-treated animals, maximal NO levels never decreased below basal concentration and on reperfusion were 100Ϯ15 nmol/L (S-NO-HSA preischemia group, 175Ϯ15 nmol/L). NO supplementation by S-NO-HSA led to partial and in the preischemia group to total preservation of high-energy phosphates and glutathione status in reperfused muscle (eg, preischemia groups: ATP, 30.23Ϯ5.02 mol/g versus control, 15.75Ϯ4.33 mol/g, PϽ0.0005; % oxidized glutathione, 4.49Ϯ1.87% versus control, 22.84Ϯ6.39%, PϽ0.0001). S-NO-HSA treatment in all groups led to protection from vasoconstriction and reduced edema formation after reperfusion (eg, preischemia groups: interfiber area, 12.94Ϯ1.36% versus control, 27.83Ϯ1.95%, PϽ0.00001). Conclusions-Long

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l -Arginine Treatment Alters the Kinetics of Nitric Oxide and Superoxide Release and Reduces Ischemia/Reperfusion Injury in Skeletal Muscle

Cited by 221 publications

References 26 publications

Race-Specific Differences in Endothelial Function

Race-Specific Differences in Endothelial Function

Localization of Inducible Nitric Oxide Synthase to Mast Cells During Ischemia/Reperfusion Injury of Skeletal Muscle

S -Nitroso Human Serum Albumin Treatment Reduces Ischemia/Reperfusion Injury in Skeletal Muscle via Nitric Oxide Release

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