Effect of Acute and Chronic N (omega)-nitro-L-arginine Administration on Plasma Nitrite/Nitrate and Malondialdehyde Levels in Rats
Abstract
Objective: The aim of this study was to investigate the effects of acute and chronic administrations of Nw nitro-L-arginine (L-NNA), a non-spesific NOS inhibitor, on plasma levels of Nitrite/Nitrate (NOx) and Malondialdehyde (MDA) in rats. Material and Method: A single dose L-NNA (aL-NNA, 25mg/kg i.p.) was administered and systolic blood pessure (SBP), NOx were measured at 1, 3, 24 hours. MDA were measured at 1, 24 hours. L-NNA was administered orally dose of 15mg/100ml/day (d-LNNA) and 45mg/100ml/day (yLNNA) for 2 weeks. dL-NNA was divided into 3 subgroups: SBP, NOx and MDA levels were determined at the end of experiments in dL-NNA0 subgroup and also 24 (dL-NNA24) and 48 hours (dL-NNA48) after the cessation of chronic L-NNA administration. yL-NNA group was not divided subgroups. Results: In the aL-NNA, SBP was higher at first and third hour which declined to the basal values at 24th hour. NOx was not change at one hour but decreased at third hour and returned to the basal levels at 24th hour. MDA were higher at first hour and remained high at 24th hour. In the long term L-NNA treated groups; both doses of L-NNA caused significant increase in SBP but NOx levels were increased only in the yL-NNA. MDA levels of dL-NNA0 were not changed but there was a significant increase in the MDA levels of the dL-NNA24, dL-NNA48 and yL-NNA. Conclusion: Results from this study indicates that acute L-NNA application causes oxidative stress but its chronic applications caused the same effect only at high doses. ©2008, Fırat University, Medical Faculty
Keywords
References
- Ellis G, Adatia I, Yazdanpanah M, Makela SK. Nitrite and nitrate analyses: a clinical biochemistry perspective. Clin Biochem 1998; 31 :195-220.
- Marzinzig M, Nussler AK, Stadler J, et al.. Improved methods to measure end products of nitric oxide in biological fluids: nitrite, nitrate, and S-nitrosothiols. Nitric Oxide 1997; 1: 177-189.
- Gardiner SM, Compton AM, Bennett T, Palmer RM, Moncada S. Control of regional blood flow by endothelium-derived nitric oxide. Hypertension 1990; 15: 486-492.
- Nagata K, Iwasaki Y, Takemura Y, et al.. Effect of inhaled NG- nitro-L-arginine methyl ester on Candida-induced acute lung injury. Chest 2003; 124: 2293-2301.
- Zatz R, Baylis C. Chronic nitric oxide inhibition model six years on. Hypertension 1998; 32 :958-964.
- Del Rio D, Stewart AJ, Pellegrini N. A review of recent studies on malondialdehyde as toxic molecule and biological marker of oxidative stress. Nutr Metab Cardiovasc Dis 2005; 15: 316-328.
- Husain K. Interaction of exercise training and chronic NOS inhibition on blood pressure, heart rate, NO and antioxidants in plasma of rats. Pathophysiology 2003; 10: 47-56.
- Cortas NK, Wakid NW. Determination of inorganic nitrate in serum and urine by a kinetic cadmium-reduction method. Clin Chem 1990; 36: 1440-1443.
- Tsaknis J, Lalas S, Tychopoulos V, Hole M, Smith G. Rapid high-performance liquid chromatographic method of determining malondialdehyde for evaluation of rancidity in edible oils. The Analyst 1998; 123: 325-327.
- Nava E, Lüscher TF. Hypertension in: Gabor M. Rubanyi (Editor) Pathophysiology and clinical application of nitric oxide. 1. Baskı, Amsterdam: Harwood Academic Publisher, 1999: 251- 266.
- Liang GY, Niu YM, Liu DX, Xu G, Cai QY. The protective efficacy of rabbit endogenous nitric oxide against acute rabbit lung ischemia-reperfusion injury and its mechanism. Sichuan Da Xue Xue Bao Yi Xue Ban. 2005; 36: 246-248.
- Wan M, Ling YL, Gu ZY, Zhang JL, Huang SS. Effects of endogenous nitric oxide on pulmonary artery hypertension and lung injury induced by endotoxin. Sheng Li Xue Bao. 1999; 51: 80-86.
- Zhang Z, Sun J, Li F, Zhang S, Cui Y, Sun H, Liu S. Protective effect of nitric oxide on pancreas and its relation to sulfhydryl compounds and oxygen free radicals. Zhonghua Wai Ke Za Zhi. 2000; 38: 928-930.
- Kilic I, Kilic BA, Güven C, Demirpence E, Aksit MA. Role of nitric oxide in hypoxia-induced changes in newborn rats. Biol Neonate 2000; 78: 191-197.
- Yin QF, Fu SH, He P, Xiong Y. Dimethylarginine dimethylaminohydrolase dimethylarginine dysfunction in rats exposed to glycosylated protein: effects of aminoguanidine. Atherosclerosis 2007; 190: 53-61. asymmetric endothelial accumulation contribute to
- Lukivskaya O, Lis R, Zwierz K, Buko V. Effect of the nitric oxide donor and the nitric oxide synthase inhibitor on the liver of rats with chronic hepatitis induced by dimethylnitrosamine. Pol J Pharmacol 2004; 56: 599-604.
- Kabul Tarihi: 03.12.2007
Akut ve Kronik N (omega)-nitro-L-arjinin Uygulamalarının Sıçanlarda Plazma Nitrit/Nitrat ve Malondialdehit Düzeylerine Etkileri
Abstract
Amaç: Bu çalışmada, sıçanlarda non-spesifik NOS inhibitörü Nw nitro-L-arjinin'in (L-NNA) akut ve kronik uygulamalarının, plazma Nitrit/Nitrat (NOx) ve Malondialdehit (MDA) düzeylerine etkilerinin araştırılması hedeflendi. Gereç ve Yöntem: Sıçanlara tek doz L-NNA (Grup aL-NNA, n=19, 25mg/kg i.p.) uygulandı; bu ana grup 3 alt gruba ayrılarak sırasıyla 1 (Grup aLNNA1, n=4), 3 (Grup aL-NNA3, n=9 ) ve 24 (Grup aL-NNA24, n=6) saat sonra sistolik kan basıncı (SKB) ve plazma NOx ölçümleri yapıldı. MDA ölçümleri ise 1. ve 24. saatlerde yapıldı. Bir diğer seri deneyde, sıçanlara iki hafta süreyle L-NNA içme suyunda iki farklı konsantrasyonda (sırasıyla, Grup dL-NNA, ≈15mg/100ml, n=19 ve Grup yL-NNA, ≈45mg/100ml, n=28) uygulandı. dL-NNA grubu 3 alt gruba ayrıldı: bir altgrupta L-NNA uygulamasının durdurulmasından hemen sonra (Grup dL-NNA0, n=7), diğerlerinde ise L-NNA uygulamasının durdurulmasından 24 (Grup dLNNA24, n=6) ve 48 (Grup dL-NNA48, n=6) saat sonra SKB, plazma NOx ve MDA düzeyleri ölçüldü. Grup yL-NNA ise altgruplara ayrılmadı. Bulgular: aL-NNA grubunda SKB 1. ve 3. saatlerde yükselirken 24.saatte bazal değerlere geri döndü. Bu grupta plazma NOx değerleri 3. saatte düştü fakat 24. saatte normale döndü, plazma MDA değerleri ise 1. saatten itibaren anlamlı şekilde yükseldi. dL-NNA0 alt grubunda deney sonunda plazma NOx ve MDA düzeyleri değişmezken dL-NNA24 ve dL-NNA48 altguplarında MDA yükseldi. yL-NNA grubunda ise hem plazma NOx hem de MDA düzeyleri yüksekti. Sonuç: Bu sonuçlar tek doz L-NNA uygulamasının oksidatif strese neden olduğunu, ancak kronik uygulamalarda oksidatif stresin sadece yüksek konsantrasyonlarda oluştuğunu göstermektedir. ©2008, Fırat Üniversitesi, Tıp Fakültesi
Keywords
References
- Ellis G, Adatia I, Yazdanpanah M, Makela SK. Nitrite and nitrate analyses: a clinical biochemistry perspective. Clin Biochem 1998; 31 :195-220.
- Marzinzig M, Nussler AK, Stadler J, et al.. Improved methods to measure end products of nitric oxide in biological fluids: nitrite, nitrate, and S-nitrosothiols. Nitric Oxide 1997; 1: 177-189.
- Gardiner SM, Compton AM, Bennett T, Palmer RM, Moncada S. Control of regional blood flow by endothelium-derived nitric oxide. Hypertension 1990; 15: 486-492.
- Nagata K, Iwasaki Y, Takemura Y, et al.. Effect of inhaled NG- nitro-L-arginine methyl ester on Candida-induced acute lung injury. Chest 2003; 124: 2293-2301.
- Zatz R, Baylis C. Chronic nitric oxide inhibition model six years on. Hypertension 1998; 32 :958-964.
- Del Rio D, Stewart AJ, Pellegrini N. A review of recent studies on malondialdehyde as toxic molecule and biological marker of oxidative stress. Nutr Metab Cardiovasc Dis 2005; 15: 316-328.
- Husain K. Interaction of exercise training and chronic NOS inhibition on blood pressure, heart rate, NO and antioxidants in plasma of rats. Pathophysiology 2003; 10: 47-56.
- Cortas NK, Wakid NW. Determination of inorganic nitrate in serum and urine by a kinetic cadmium-reduction method. Clin Chem 1990; 36: 1440-1443.
- Tsaknis J, Lalas S, Tychopoulos V, Hole M, Smith G. Rapid high-performance liquid chromatographic method of determining malondialdehyde for evaluation of rancidity in edible oils. The Analyst 1998; 123: 325-327.
- Nava E, Lüscher TF. Hypertension in: Gabor M. Rubanyi (Editor) Pathophysiology and clinical application of nitric oxide. 1. Baskı, Amsterdam: Harwood Academic Publisher, 1999: 251- 266.
- Liang GY, Niu YM, Liu DX, Xu G, Cai QY. The protective efficacy of rabbit endogenous nitric oxide against acute rabbit lung ischemia-reperfusion injury and its mechanism. Sichuan Da Xue Xue Bao Yi Xue Ban. 2005; 36: 246-248.
- Wan M, Ling YL, Gu ZY, Zhang JL, Huang SS. Effects of endogenous nitric oxide on pulmonary artery hypertension and lung injury induced by endotoxin. Sheng Li Xue Bao. 1999; 51: 80-86.
- Zhang Z, Sun J, Li F, Zhang S, Cui Y, Sun H, Liu S. Protective effect of nitric oxide on pancreas and its relation to sulfhydryl compounds and oxygen free radicals. Zhonghua Wai Ke Za Zhi. 2000; 38: 928-930.
- Kilic I, Kilic BA, Güven C, Demirpence E, Aksit MA. Role of nitric oxide in hypoxia-induced changes in newborn rats. Biol Neonate 2000; 78: 191-197.
- Yin QF, Fu SH, He P, Xiong Y. Dimethylarginine dimethylaminohydrolase dimethylarginine dysfunction in rats exposed to glycosylated protein: effects of aminoguanidine. Atherosclerosis 2007; 190: 53-61. asymmetric endothelial accumulation contribute to
- Lukivskaya O, Lis R, Zwierz K, Buko V. Effect of the nitric oxide donor and the nitric oxide synthase inhibitor on the liver of rats with chronic hepatitis induced by dimethylnitrosamine. Pol J Pharmacol 2004; 56: 599-604.
- Kabul Tarihi: 03.12.2007
Details
| Primary Language | Turkish |
|---|---|
| Journal Section | Articles |
| Authors | |
| Publication Date | April 1, 2008 |
| Published in Issue | Year 2008 Volume: 13 Issue: 2 |