曲美他嗪和维生素e作为环孢素a毒性药物保护剂的性能研究。

ISRN Pharmacology Pub Date : 2013-04-11 Print Date: 2013-01-01 DOI:10.1155/2013/605640
De la Cruz Rodríguez Lilia Cristina, Rey María Del Rosario, Araujo Carmen Rosa, Oldano Ana Veronica
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引用次数: 7

摘要

免疫抑制剂环孢素A (cyclosporin A, CyA)已广泛应用于有免疫学基础的疾病和移植患者。肾毒性和肝毒性是该药的主要不良反应。为了找到一种对抗这些影响的保护药物,我们测试了心脏保护剂曲美他嗪(TMZ)和维生素E,它们被用作缓解氧化应激的营养补充剂。取雄性Wistar大鼠6组,每组8只(A- f组):A,对照组;B、维生素E(10毫克/公斤/天);C、TMZ (20 mg/Kg/天);D, 25 mg/Kg/天CyA;E、CyA和维生素E(25毫克/公斤/天CyA + 10毫克/公斤/天维生素E);F、TMZ 20天(20 mg/kg/天);其次是CyA (25 mg/kg/d)和TMZ (20 mg/kg/d)。试验期120 d。大鼠暴露于CyA后,血清尿素、肌酐和谷氨酸脱氢酶(GLDH)升高,促进肾毒性和肝毒性。对肝脏和肾脏进行了结构和超微结构研究。与对照组(A)相比,D组出现CyA诱导的不良反应,差异有统计学意义。维生素E (E)无保护作用。TMZ (F)预处理可减轻CyA的不良反应。我们认为,TMZ的细胞保护作用可以减轻cya引起的肾毒性和肝毒性。TMZ抑制重吸收,从而抑制CyA在细胞中的积累。维生素E的抗氧化能力并没有提高CyA的抗氧化效果。
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On the performance of trimetazidine and vitamin e as pharmacoprotection agents in cyclosporin a-induced toxicity.

The immunosuppressant drug cyclosporin A (CyA) has been used in diseases with immunological basis and in transplant patients. Nephrotoxicity and hepatotoxicity are the main adverse effects of this drug. To find a protective drug against those effects we assayed the cardioprotector Trimetazidine (TMZ) and vitamin E, used as nutritional supplements to alleviate oxidative stress. Six groups of eight male Wistar rats each were prepared (groups A-F): A, control; B, vitamin E (10 mg/Kg/day); C, TMZ (20 mg/Kg/day); D, 25 mg/Kg/day CyA; E, CyA and vitamin E (25 mg/Kg/day CyA + 10 mg/Kg/day Vit E); F, TMZ for 20 days (20 mg/kg/day); and then CyA (25 mg/kg/day) and TMZ (20 mg/Kg/day). The experiment lasted 120 days. The exposure of rats to CyA promoted nephrotoxicity and hepatotoxicity with an increase in serum urea, creatinine, and glutamate dehydrogenase (GLDH). Structural and ultrastructural studies of liver and kidney were performed. Group D showed adverse effects induced by CyA since statistically significant differences were found with respect to the control group (A). Vitamin E (E) showed no protective effect. Pretreatment with TMZ (F) attenuated the adverse effects of CyA. We conclude that CyA-induced nephrotoxicity and hepatotoxicity are attenuated by the cytoprotective effect of TMZ. TMZ inhibits the reabsorption and, consequently, the accumulation of CyA in the cell. The antioxidant capacity of vitamin E did not improve the effect of CyA.

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