Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats

ÇİÇEK, Ekrem; GÖKÇİMEN, Aparslan; GÖKALP, Osman; KARAHAN, NERMİN; AYDIN, Gülsen; ÖNCÜ, Meral

Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats

Gülsen AYDIN, (Süleyman Demirel Üniversitesi, Tıp Fakültesi, Isparta, Türkiye)

Aparslan GÖKÇİMEN, (Girilmedi)

Meral ÖNCÜ, (Girilmedi)

Ekrem ÇİÇEK, (Girilmedi)

Nermin KARAHAN, (Girilmedi)

Osman GÖKALP (Girilmedi)

Turkish Journal of Veterinary and Animal Sciences

4 0

Yıl: 2003 Cilt: 27 Sayı: 5 Sayfa Aralığı: 1131 - 1140 Metin Dili: Türkçe İndeks Tarihi: 29-07-2022

Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats

Öz:

: Non-steroidal anti-inflamatuar ilaçlar (NSAIDs) dünyada yaygın olarak kullanılırlar. Bu ilaçlar bazen yalnışlıkla yüksek ya da toksik dozda kullanılabilirler. Bu çalışmada, farklı dozlarda diclofenac sodium'un karaciğer ve böbrek dokuları üzerine etkilerini araştırmayı amaçladık. Wistar Strain cinsi ağırlıkları 200-220 gram olan 40 adet olgun Albino ratlar, her biri l O rattan oluşan 4 gruba ayrıldı. Kontrol grubu olan ratlara (n = 10) intramüsküler olarak l cc serum fizyolojik enjekte edildi. Diğer üç gruba diclofenac sodium'un farklı dozları'uygulandı. Birinci (n = 10), ikinci (n = 10) ve üçüncü (n = 10) grup ratlara 5 gün süre ile hergün 50, 100, 150 mg/kg, düşük, orta ve yüksek dozlarda diclofenac sodium intramüsküler olarak enjekte edildi. Beş günlük deney süresi sonunda hayvanlar ötenazi edildikten sonra nekropsileri yapılarak, karaciğer ve böbrek doku örnekleri histopatolojik inceleme için hazırlandı. Kontrol grubu ratların karaciğer ve böbrek dokularının histopatolojik incelenmesinde önemli değişiklikler gözlenmedi (P > 0,05). Diclofenac sodium tedavisi, karaciğer ve böbrek dokularını önemli derecede etkiledi (P < 0,001). Diclofenac tedavili bütün grupların, hematoksilen-eosin ile boyalı karaciğer kesitlerindeki histopatolojik değişiklikler: Karaciğer hücrelerinde bulanık şişkinlik ve hidropik dejenerasyon, fokal sinusoidal ve santral ven genişlemesi, portal alanlarda safra kanal proliferasyonu, mononükleer hücreînfiltrasyonu ile birlikte periportal mesafe genişlemesi, hiperemi, fokal nekrozlar ve doza bağlı fıbröz doku artışıydı. Diclofenac sodium tedavili bütün grupların böbrek dokularının tübüler epitel hücrelerinde bulanık şişkinlik ve hidropik dejenerasyon görüldü. Fakat, nekroz, peritübüler lenfosit infıltrasyonu, interstisiyumda fibröz doku artışı, hiperemi ikinci ve üçüncü gruplarda gözlendi. Yüksek doz diclofenac sodium verilen üçüncü grubun karaciğer ve böbrek dokularında görülen nekroz, hidropik dejenerasyon ve inflamasyon, düşük dozla karşılaştırıldığında, daha yaygın ve yoğun idi. Böbrek dokusunda ve karaciğerin periportal alanlarında düzensizliğe neden olan bağ dokusu artışı sadece yüksek doz alan grupta görüldü. Bu bulgular, yüksek doz diclofenac sodium'un karaciğer ve böbrek dokularında anlamlı değişikliklere neden olduğunu göstermektedir.

Anahtar Kelime: karaciğer böbrekler diklofenak sodyum doku kültürü histopatoloji sıçan

Konular: Ziraat Mühendisliği

Farklı dozlarda diclofenac sodium'un ratların karaciğer ve böbrek dokusunda oluşturduğu histopatolojik değişiklikler

Öz:

: Non-steroidal anti-inflammatory drugs (NSAIDs) are in common use worldwide. These drugs may sometimes be used in high or toxic doses by mistake. In this study we investigated the effects of different doses of diclofenac sodium on liver and renal tissues. Forty albino adult male Wistar rats weighing 200 to 220 g were divided equally into four groups. The rats in the control group (n = 10) were each intramuscularly injected with 1 cc of physiologic saline. The other three groups were given diclofenac sodium doses. The rats in the first (n = 10), second (n = 10) and third (n = 10) groups were intramuscularly injected with diclofenac sodium at a low, medium and high dose of 50, 100 and 150 mg/kg live weight/day, respectively, every day for 5 days. At the end of the experimental period (5 days), after the animals were sacrificed, they were autopsied and liver and kidney tissue samples were prepared for histopathologic assessment. No significant (P > 0.05) changes were observed in the histopathology of the liver or kidney tissues of the control rats. The diclofenac sodium treatment significantly (P < 0.001) affected the histopathology of both the liver and kidney. Histopathologic changes in the liver sections stained with hematoxylin and eosin in all diclofenac groups included claudy swelling and hydropic degeneration of the liver cells, focal sinusoidal and vena centralis dilatation, proliferation of the bile duct in portal areas, enlargement of the periportal area with mononuclear cell infiltration, hyperemia and dose-dependent fibrous tissues proliferation and focal necrosis. Cloudy swelling and hydropic degeneration were seen in the tubular epithelial cells of the kidney tissue of all diclofenac sodium treated groups. Necrosis, peritubular lymphocyte infiltration, stromal fibrous tissue proliferation and hyperemia were observed in the second and third groups. In the liver and kidney tissue of the third group, which was given a high dose of diclofenac sodium, necrosis, cloudy swelling and hydropic degeneration and inflammation were rather widespread and intensive, as compared to the group given a low dose. The increase in fibrous tissue in the kidney and liver that caused irregularities in the periportal areas was only seen in the group given a high dose. These results suggest that a high dose of diclofenac sodium causes meaningful changes in liver and kidney tissue.

Anahtar Kelime: histopathology rats liver kidneys diclofenac sodium tissue culture

Konular: Ziraat Mühendisliği

Belge Türü: Makale Makale Türü: Araştırma Makalesi Erişim Türü: Erişime Açık

Radwan, M.A.: Zidovudine, diclofenac and ketoprofen pharmacokinetic interactions in rats.: J. Pharm. Pharmacol., 2000:52:665-669.
Simon, L.S.: Actions and toxic effects of the nonsteroidal anti- inflammatory drugs. Curr. Opin. Rheumatol., 1994; 6: 238-251.
Manoukian, A.V., Carson, J.L.: Nonsteroidal anti-inflammatory drug-induced hepatic disorders. Incidence and prevention. Drug Saf., 1996; 15:64-71.
Skoutakis, V.A., Carter, C.A., Mickle, T.R., Smith, V.H., Arkin, C.R., Alissandratos, J., Petty, D.E.: Review of diclofenac and evaluation of its place in therapy as a nonsteroidal antiinflammatory agent. Drug Intell. Clin. Pharm, 1988; 22: 850-859.
Rubatelli, F.F., Chiozza, M.L., Zanardo, V., Cantrutti, F.: Effect on neonate of maternal treatment with indomethacin. J. Pediatr., 1979:94:161-165.
Kayaalp, S.O.: Rasyonel tedavi yönünden tıbbi farmakoloji. Medicine Pharmacology. 8. baskı. Ankara., Hacettepe Taş Kitapçılık, Ltd. Şti., pp. 1032-1046, 1998.
Gettigan, M. P., Henry, D.: Current problems with non-specific COX inhibitors. Curr. Pharm. Des., 2000; 6: 1693-1724.
Menasse, R., Hedwall, P.R., Kraetz, J., Pericin, C, Riesterer, L, Sallmann, A., Ziel; R., Jaques, R.: Pharmacological properties of diclofenac sodium and its metabolites. Scand. J. Rheumatol. Suppl., 1978; 22:5-16.
Zaragoza, M. A., Alfonso, M.V., Roig, C.E.: NSAID-induced hepatotoxicity: aceclofenac and diclofenac. Rev. Esp. Enferm. Dig., 1995:87:472-475.
Goodman and Gilman's.: Diclofenac Sodium. The Pharmacological Basic of Therapeutics. Ninth Edition. New York., p.: 637, 1995.
Castel, J.V., Gomez-Lechon, M.J., Ponsoda, X., Bort, R .: The use of cultured hepatocytes to investigate the mechanism of drug hepatotoxicity. Cell Biol. Toxicol., (Review), 1997; 13: 331-338.
Gökçimen, A., Aydın, G., Karaöz, E, Malas, M.A., Öncü, M.: Effect of diclofenac sodium administration during pregnancy in the postnatal period. Fetal Diagn. Ther., 2001; 16: 417-422.
Gökçimen, A., Akdoğan, M., Karaöz, E.: Structural and biochemical changes in liver and renal tissues induced by an acute high dose of diclofenac sodium in rats. Biomed. Res., 2000; 11: 293-302.
Kertz-Rommel, D.A., Boelsteri, U.A.: Diclofenac covalent protein binding is dependent on acyl glucuronide formation and is inversely related to P 450-mediated acute cell injury in cultured rat hepatocytes. Toxicol. Appl. Pharmacol., 1993; 120: 155-161.
Hargus, S.J., Amouzedeh, H.R., Pumford, N.R.: Metabolic activation and immunochemical localization of liver protein adducts of the nonsteroidal anti-inflammatory drug diclofenac. Chem. Res. Toxicol., 1994; 7: 575-582.
Tolman, K.G': Hepatotoxicity of non-narcotic analgesics. Am. J. Med., (Review)., 1998; 105: 13Ş-19S.
Castel, J.V., Gomez-Lechon, M.J., Ponsoda, X., Bort, R.: The use of cultured hepatocytes to investigate the mechanism of drug hepatotoxicity. Cell Biol. Toxicol., 1997; 13: 33Î-338.
Dunk, A.A., Walt, R.P., Jenkins, W.J., Sherlock, S.S.: Diciofenac hepatitis. Br. Med. J., 1982; 284: 160-166.
Sergio, A.U., Antonio, C.S.: Diciofenac sodium and mefenamic acid: Potent inducers of the membrane permeability transition in renal cortex mitochondria. Arch. Biochem. Biophys., 1997; 342: 231-235.
Moreno-Sanchez, R., Bravo, C, Vasquez, C, Ayala, G., Silveira, L.H., Martinez-Lavin, M.: Inhibition and uncoupling of oxidative phosphorylation by nonsteroidal anti-inflammatory drugs: Study in mitochondria, submitochondrial particles, cells, and whole heart. Biochem. Pharmacol., 1999; 57: 743-752.
Bort, R., Ponsoda, X., Jover, R., Gomez-Lechon, M.J., Castell, J.V.: Diciofenac toxicity to hepatocytes: A role for drug metabolism in cell toxicity. J. Pharmacol. Exp. Ther., 1999; 288: 65-72.
Brune, K., Lindner, J.: Side effects of anti-inflammatory drugs. In: Inflammation and Drug Therapy Series, 1992; 5: 198-203.
Kappus, H.: Overview of enzyme systems involved in bioreduction of drugs and redox cycling. Biochem. Pharmacol., 1986; 35: 1-6.
Tang, W., Stearns, R.A., Bandiera, S.M., Zhang, Y., Raab, C, Braun, M.P., Dean, D.C., Pang, J., Leung, K.H., Doss, G.A., Strauss, J.R., Kwei, G.Y., Rushmore, T.H., Chiu, S.H., Baillie, T.A.: Studies on cytochrome P-450-mediated bioactivation of diciofenac in rats and in human hepatocytes: Identification of glutathione conjugated metabolites. Drug Metab. Dispos., 1999; 27: 365-372.
Farrell, G.C.: Drug-induced hepatic injury. J. Gastroenterol. Hepatol., 1997; 12: 242-250.
Akdoğan, M., Akkuş, S.: Investigation of erythrocyte antioxidant enzymes activities in high dose diciofenac sodium applied rats. Biomed. Res., 2001; 12: 53-57.
Clive, D.M., Stoff, J.S.: Renal syndromes associated with nonsteroidal anti-inflammatory drugs. N. Engl. J. Med., 1984; 310:563-572.
Murray, M.D., Brater, D.C.: Renal toxicity of nonsteroidal anti- inflammatory drugs. Annu. Rev. Pharmacol. Toxicol., 1993; 32: 435-465.
Palmer, B.F.: Renal complications associated with use of nonsteroidal anti-inflammatory agents. J. Invest. Med., 1995; 43: 516-553.
Abromson, S.B., Weissmann, G.: The mechanism, of action of nonsteroidal anti-inflammatory drugs. Arth. Rheum., 1988; 32:1.
Lowry, O.H., Rosebrough, N.J., Randall, R.J.: protejn measurement with the Folin phenol reagent. J. Biol. Chem 1951:182:265-268.
Anderson, H.C., Chen, H., Pellet, L.T., Tappel, A.L.: Ferous-ir0n. induced oxidation in chicken liver slices as measured bv hemichrome formation and thiobarbituric acid reactive substances: Effect of dietary vitamin E and beta-carotene. Free Radic. Biol. Med., 1993; 15: 35-48.
Aebi, H.: Catalase. Methods of enzymatic analysis, in Beregmeyer, H.U., London, New York, Academic Press, p. 673, 1974.
Schmitz, G., Lepper, H., Estler, C.J.: Changes in energy homeostasis and GSH-depletion as possible mechanisms of diciofenac induced cytotoxicity on isolated rat hepatocytes. Naunyn Schmied Eberas. Arch. Pharmacol., 1995; 77: 32-35.
Babany, G., Bernuau, J., Danan, G., Rueff, B., Benhamou, J.p. Hepatite fulminante chez une femme prenant de la glafenine et du dislofenac. Gastroenterol. Clin. Biol., 1985; 9: 185.
Castot, A., Netter, P., Arnaudo, J.P.: Pirprofen induced hepatitis with favourable outcome. Therapie, 1984; 3: 297-303.
Radford, M.G. Jr., Holley, K.E., Grande, J.P., Larson, T.S., Wagoner, R.D., Donadio, J.V., McCarthy, J.T.: Reversible membranous nephropathy associated with the use of nonsteroidal anti-inflammatory drugs. J. Am. Med. Assoc, 1996; 276: 466-469.
Hunter, D.R., Haworth, R.A.: The Ca2+ induced membrane transition in mitochondria. I. The protective mechanisms. Arch. Biochem. Biophys, 1979; 195: 453-459.
Castilho, R.F., Kowaltowski, A.J., Meinjcke, Permeabilization of the inner mitochondrial membrane by Ca ions is stimulated byt-butyl hydroperoxide and mediated by reactive oxygen species generated by mitochondria. Free Radical. Biol. Med., 1995; 18:479-486.
Kawaltovski, A.J., Castilho, R.F.: Opening of the mitochondrial permeability transition pro by uncoupling or inorganic phosphate in the presence of Ca2+ is dependent on mitochondrial generated reactive oxygen species. FEBS Lett, 1996; 378: 150-152.
Bernardi, P., Broekemeier, K.M., Pfeiffer, D.R.: Recent progress on regulation of the mitochondrial permeability transition pore, a cyclosporin-sensitive pore in the inner mitochondrial membrane ; J. Bioenerg. Biomembr., 1994; 26: 509-517.
Mingatto, F.E., Santor, A.C., Uyemura, S.A.: In vitro interaction of nonsteroidal anti-inflammatory drugs on oxidative phosphorylation of rat. Arch. Biochem. Biophy., 1996; 334: SOS- SOS.

APA	AYDIN G, GÖKÇİMEN A, ÖNCÜ M, ÇİÇEK E, KARAHAN N, GÖKALP O (2003). Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats. , 1131 - 1140.
Chicago	AYDIN Gülsen,GÖKÇİMEN Aparslan,ÖNCÜ Meral,ÇİÇEK Ekrem,KARAHAN NERMİN,GÖKALP Osman Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats. (2003): 1131 - 1140.
MLA	AYDIN Gülsen,GÖKÇİMEN Aparslan,ÖNCÜ Meral,ÇİÇEK Ekrem,KARAHAN NERMİN,GÖKALP Osman Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats. , 2003, ss.1131 - 1140.
AMA	AYDIN G,GÖKÇİMEN A,ÖNCÜ M,ÇİÇEK E,KARAHAN N,GÖKALP O Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats. . 2003; 1131 - 1140.
Vancouver	AYDIN G,GÖKÇİMEN A,ÖNCÜ M,ÇİÇEK E,KARAHAN N,GÖKALP O Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats. . 2003; 1131 - 1140.
IEEE	AYDIN G,GÖKÇİMEN A,ÖNCÜ M,ÇİÇEK E,KARAHAN N,GÖKALP O "Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats." , ss.1131 - 1140, 2003.
ISNAD	AYDIN, Gülsen vd. "Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats". (2003), 1131-1140.

APA	AYDIN G, GÖKÇİMEN A, ÖNCÜ M, ÇİÇEK E, KARAHAN N, GÖKALP O (2003). Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats. Turkish Journal of Veterinary and Animal Sciences, 27(5), 1131 - 1140.
Chicago	AYDIN Gülsen,GÖKÇİMEN Aparslan,ÖNCÜ Meral,ÇİÇEK Ekrem,KARAHAN NERMİN,GÖKALP Osman Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats. Turkish Journal of Veterinary and Animal Sciences 27, no.5 (2003): 1131 - 1140.
MLA	AYDIN Gülsen,GÖKÇİMEN Aparslan,ÖNCÜ Meral,ÇİÇEK Ekrem,KARAHAN NERMİN,GÖKALP Osman Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats. Turkish Journal of Veterinary and Animal Sciences, vol.27, no.5, 2003, ss.1131 - 1140.
AMA	AYDIN G,GÖKÇİMEN A,ÖNCÜ M,ÇİÇEK E,KARAHAN N,GÖKALP O Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats. Turkish Journal of Veterinary and Animal Sciences. 2003; 27(5): 1131 - 1140.
Vancouver	AYDIN G,GÖKÇİMEN A,ÖNCÜ M,ÇİÇEK E,KARAHAN N,GÖKALP O Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats. Turkish Journal of Veterinary and Animal Sciences. 2003; 27(5): 1131 - 1140.
IEEE	AYDIN G,GÖKÇİMEN A,ÖNCÜ M,ÇİÇEK E,KARAHAN N,GÖKALP O "Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats." Turkish Journal of Veterinary and Animal Sciences, 27, ss.1131 - 1140, 2003.
ISNAD	AYDIN, Gülsen vd. "Histopatological changes in liver and renal tissues induced by different doses of diclofenac sodium in rats". Turkish Journal of Veterinary and Animal Sciences 27/5 (2003), 1131-1140.