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Literature DB >> 12701821

Role of nitric oxide synthase activity in experimental ischemic acute renal failure in rats.

Mild Komurai¹, Yasuko Ishii, Fumiaki Matsuoka, Katsuhide Toyama, Masayuki Ominato, Takeo Sato, Teruhiko Maeba, Kenjiro Kimura, Shigeru Owada.

Abstract

To determine the role of nitric oxide (NO) in acute renal failure (ARF), we have studied the time course change activities to activity of nitric oxide synthase (NOS) isoform activities, both calcium dependent and independent NOS, in experimental ischemic ARF. We have also analyzed change activities to activity of the NOS activities in both renal cortex and medulla. Male SD rats (n = 5) were inducted to ARF by ischemia-reperfusion injury and divided into the following groups; Control group (sham operation), Day 0 group, (measurement performed on that day of operation), Day 1 group, (measurement performed one day after induction of ARF), Day 3 group and Day 7 group. Measurement of NOS activity was based on the following principles; NO is synthesized from arginine by nitric oxide synthase (NOS) and NO is converted to NO2(-)/NO3(-)(NOx) by oxidation. Detection of the final metabolite of NO, NOx was done using flow injection method (Griess reaction). The results were, (1) calcium dependent NOS activity in the cortex and medulla decreased, however it increased in the recovery period in the renal cortex (Cortex; Control, 0.941 +/- 0.765, D0, 0.382 +/- 0.271, D1, 0.118 +/- 0.353, D3, 2.030 +/- 0.235, D7, 3.588 +/- 2.706, Medulla; Control, 1.469 +/- 0.531, D0, 0.766 +/- 0.156, D1, 0.828 +/- 0.187, D3, 2.078 +/- 0.094, D7, 1.289 +/- 0.313 micromol NOx produced/mg protein/30 min). (2) On the other hand, iNOS activity increased in the early phase of ARF, both in the cortex and medulla, but returned to control values during the recovery phase in cortex and was maintained at higher levels in the medulla (Cortex; Control, 0.333 +/- 0.250, D0, 0.583 +/- 0.428, D1, 1.167 +/- 0.262, D3, 0.250 +/- 0.077, D7, 0.452 +/- 0.292, Medulla; Control, 0.139 +/- 0.169, D0, 0.279 +/- 0.070, D1, 1.140 +/- 0.226, D3, 0.452 +/- 0.048, D7, 0.625 +/- 0.048 micromol NOx produced/mg protein/30 min). These findings suggest that the role of NOS in ARF are different for the different NOS isoforms and have anatomic heterogeneity.

Entities: Chemical Disease Species

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Year: 2003 PMID： 12701821

Source DB: PubMed Journal: Mol Cell Biochem ISSN： 0300-8177 Impact factor: 3.396

17 in total

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Review 2. Nitric oxide in renal health and disease.

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Authors: J S Beckman; T W Beckman; J Chen; P A Marshall; B A Freeman
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5. Decline in the expression of copper/zinc superoxide dismutase in the kidney of rats with endotoxic shock: effects of the superoxide anion radical scavenger, tempol, on organ injury.

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2. Rosiglitazone affects nitric oxide synthases and improves renal outcome in a rat model of severe ischemia/reperfusion injury.

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2 in total

Role of nitric oxide synthase activity in experimental ischemic acute renal failure in rats.

1. Analysis of nitrite, nitrate, and nitric oxide synthase activity in brain tissue by automated flow injection technique.

Review 2. Nitric oxide in renal health and disease.

3. L-arginine reduces tubular cell injury in acute post-ischaemic renal failure.

4. Apparent hydroxyl radical production by peroxynitrite: implications for endothelial injury from nitric oxide and superoxide.

5. Decline in the expression of copper/zinc superoxide dismutase in the kidney of rats with endotoxic shock: effects of the superoxide anion radical scavenger, tempol, on organ injury.

Review 6. Therapeutic strategies in the prevention of acute renal failure.

Review 7. Biology of ischemic and toxic renal tubular cell injury: role of nitric oxide and the inflammatory response.

8. In vivo targeting of inducible NO synthase with oligodeoxynucleotides protects rat kidney against ischemia.

9. Nitric oxide kinetics during hypoxia in proximal tubules: effects of acidosis and glycine.

10. Hypoperfusion-induced acute renal failure in the rat: an evaluation of oxidant tissue injury.

1. Induction of proinflammatory cytokines and nitric oxide by Trypanosoma cruzi in renal cells.

2. Rosiglitazone affects nitric oxide synthases and improves renal outcome in a rat model of severe ischemia/reperfusion injury.