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      Atorvastatin Has no Effects on Kidney Tissues of Wistar Albino Rats in the Long-Term Intake: An Electron Microscopic Study Translated title: Atorvastatina no Tiene Efectos sobre los Tejidos Renales de Ratas Wistar Albinas en el Consumo a Largo Plazo: Un Estudio de Microscopia Electrónica

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          Abstract

          In this study, we evaluated the ultrastructural findings of kidney with systemic administration of different doses of atorvastatin in a rat model. Statins may have anti-inflammatory effects that would play a role in preventing the cellular damage. The aim of this study was to investigate how atorvastatin could play a role in kidney tissues. Forty adult male Wistar albino rats (200250 g) were randomly divided into 4 groups of ten rats each (A1, A2, A3 and Control). Three different doses of atorvastatin were used to determine the effects on kidney tissues during 90 day period. The kidneys of A1 (0.1-mg group), A2 (0.5-mg group) and A3 (1-mg group) group were excised and the tissues were examined after the 90 days by transmission electron microscopy. Despite increasing the dose of atorvastatin intake, the histological structures of atorvastatin groups were appeared normal in the same period. In conclusion, long-term use of atorvastatin was not found to have an adverse effect on kidney tissue.

          Translated abstract

          En un modelo de rata, se evaluaron los hallazgos ultraestructurales del riñón provocados por la administración sistémica de diferentes dosis de atorvastatina. Las estatinas pueden tener efectos anti-inflamatorios que desempeñan un importante rol en la prevención del daño celular. El objetivo de este estudio fue investigar cómo la atorvastatina podría desempeñar un papel en los tejidos del riñón. 40 Ratas Wistar albinas Adultas (200-250 g) machos fueron divididas aleatoriamente en cuatro grupos de 10 ejemplares cada uno (A1, A2, A3 y Control). Tres diferentes dosis de atorvastatina se utilizaron para determinar los efectos sobre los tejidos del riñón durante un período de 90 días. Los riñones de los grupos A1 (0,1 mg), A2 (0,5 mg) y A3 (1 mg) fueron extirpados a los 90 días y los tejidos examinados por microscopía electrónica de transmisión. A pesar de haberse aumentado la dosis de ingesta de atorvastatina, las estructuras histológicas se asemejaron al grupo normal del mismo período. En conclusión, el uso de atorvastatina en un plazo prolongado, no produce efecto negativo sobre el tejido renal.

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          The effect of pravastatin on coronary events after myocardial infarction in patients with average cholesterol levels. Cholesterol and Recurrent Events Trial investigators.

          Frank Sacks, Marc Pfeffer, Lemuel Moyé (1996)
          In patients with high cholesterol levels, lowering the cholesterol level reduces the risk of coronary events, but the effect of lowering cholesterol levels in the majority of patients with coronary disease, who have average levels, is less clear. In a double-blind trial lasting five years we administered either 40 mg of pravastatin per day or placebo to 4159 patients (3583 men and 576 women) with myocardial infarction who had plasma total cholesterol levels below 240 mg per deciliter (mean, 209) and low-density lipoprotein (LDL) cholesterol levels of 115 to 174 mg per deciliter (mean, 139). The primary end point was a fatal coronary event or a nonfatal myocardial infarction. The frequency of the primary end point was 10.2 percent in the pravastatin group and 13.2 percent in the placebo group, an absolute difference of 3 percentage points and a 24 percent reduction in risk (95 percent confidence interval, 9 to 36 percent; P = 0.003). Coronary bypass surgery was needed in 7.5 percent of the patients in the pravastatin group and 10 percent of those in the placebo group, a 26 percent reduction (P=0.005), and coronary angioplasty was needed in 8.3 percent of the pravastatin group and 10.5 percent of the placebo group, a 23 percent reduction (P=0.01). The frequency of stroke was reduced by 31 percent (P=0.03). There were no significant differences in overall mortality or mortality from noncardiovascular causes. Pravastatin lowered the rate of coronary events more among women than among men. The reduction in coronary events was also greater in patients with higher pretreatment levels of LDL cholesterol. These results demonstrate that the benefit of cholesterol-lowering therapy extends to the majority of patients with coronary disease who have average cholesterol levels.
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            Effect of intensive lipid lowering with atorvastatin on renal function in patients with coronary heart disease: the Treating to New Targets (TNT) study.

            Andrei Breazna, James Shepherd, Jonathan J. Wilson (2007)
            Data suggest that atorvastatin may be nephroprotective. This subanalysis of the Treating to New Targets study investigated how intensive lipid lowering with 80 mg of atorvastatin affects renal function when compared with 10 mg in patients with coronary heart disease. A total of 10,001 patients with coronary heart disease and LDL cholesterol levels of or = 60 ml/min per 1.73 m2 in significantly more patients and declined to < 60 ml/min per 1.73 m2 in significantly fewer patients than in the 10-mg arm. The expected 5-yr decline in renal function was not observed. Estimated GFR improved in both treatment groups but was significantly greater with 80 mg than with 10 mg, suggesting this benefit may be dosage related.
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              Renal injury of diet-induced hypercholesterolemia in rats.

              Bertram Kasiske, Michael P O'Donnell, Paul G Schmitz (1990)
              Abnormalities in lipid metabolism frequently accompany renal disease and may be important in the pathogenesis of progressive renal injury. In the present study, the effects of a high cholesterol diet on renal histology, cortical lipids, and glomerular hemodynamic function were examined in normal rats with and without reduced renal mass. Cholesterol feeding for 19 weeks increased serum cholesterol from 66 +/- 10 mg/dl to 256 +/- 93 mg/dl in two-kidney rats, and from 73 +/- 15 mg/dl to 407 +/- 274 mg/dl in nephrectomy rats (P less than 0.01). Both sham-operated and unilateral nephrectomy rats fed a high cholesterol diet had a greater amount of glomerulosclerosis and tubulointerstitial damage than rats fed standard chow. Cortical cholesteryl esters were increased by the cholesterol diet, and correlated with the amount of glomerulosclerosis (r = 0.90, P less than 0.01) and tubulointerstitial injury (r = 0.64, P less than 0.05). Cholesterol feeding and nephrectomy both caused alterations in tissue essential fatty acids, and a panel of specific monoclonal antibodies indicated that renal injury and cortical lipid alterations were associated with an increase in glomerular macrophages. Finally, micropuncture experiments carried out in a separate group of rats fed high cholesterol for 8 to 10 weeks demonstrated increases in glomerular capillary pressure. These results suggest that additional investigations may ultimately determine how cholesterol deposition, altered fatty acid metabolism, macrophages, and increased glomerular pressure might combine to cause chronic progressive renal injury.
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                Author and article information

                Journal
                Journal ID (publisher-id): ijmorphol
                Title: International Journal of Morphology
                Abbreviated Title: Int. J. Morphol.
                Publisher: Sociedad Chilena de Anatomía (Temuco, , Chile )
                ISSN (Electronic): 0717-9502
                Publication date (Print and electronic): March 2011
                Volume: 29
                Issue: 1
                Pages: 144-150
                Affiliations
                [03] Izmir orgnameDokuz Eylül University orgdiv1Faculty of Medicine orgdiv2Department of Histology and Embryology Turkey
                [02] Diyarbakir orgnameDicle University orgdiv1Faculty of Medicine orgdiv2Department of Anatomy Turkey
                [01] Diyarbakir orgnameDicle University orgdiv1Faculty of Medicine orgdiv2Department of Histology and Embryology Turkey
                Article
                Publisher ID: S0717-95022011000100025 Publisher ID: S0717-9502(11)02900125
                DOI: 10.4067/S0717-95022011000100025
                SO-VID: 3fcc5e5e-ae5c-4668-bc3e-8be0e2434189
                License:

                This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License.

                History
                Date accepted : 19 November 2010
                Date received : 24 September 2010
                Page count
                Figures: 0, Tables: 0, Equations: 0, References: 43, Pages: 7
                Product

                SciELO Chile


                Keywords: Ultrastructural,Kidney,Wistar-albino rat,Statins,Atorvastatin,Riñón,Ratas Wistar albinas,Estatinas,Atorvastatina,Ultraestructurales
                Data availability:
                Keywords: Ultrastructural, Kidney, Wistar-albino rat, Statins, Atorvastatin, Riñón, Ratas Wistar albinas, Estatinas, Atorvastatina, Ultraestructurales

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