Evaluation of the effect of administration of Tadalafil on Gentamicin-induced nephrotoxicity in rats

Egyptian Journal of Medical Research Pub Date : 2022-10-01 DOI:10.21608/ejmr.2022.267691

Ekhlas A. I. Mohammed, A. Elberry, Marwa Sayed, Sherif Abdelfatah

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引用次数: 1

Abstract

: Background: Gentamicin (GNT) is a highly effective aminoglycoside antibiotic that is commonly used to treat life-threatening bacterial infections. Aim: The aim of the current study is to determine whether tadalafil can protect against GNT-induced nephrotoxicity. Methods: Twenty-four male Albino rats were used in the study, which were randomly divided into four groups, six animals each. Control untreated group received distilled water (5ml/kg, P.O) for 12 days and on days 6-12, they received (5ml/kg,i.p) normal saline daily, one hour after oral administration of distilled water. Tadalafil group received tadalafil (5mg/kg, P.O) for 12 days and on days 6-12, they received (5ml/kg,i.p) of normal saline daily, one hour after oral administration of tadalafil. Gentamicin group received distilled water (5ml/kg, P.O) and on days 6-12, they received gentamicin (011mg/kg,i.p) one hour after oral administration of distilled water. Gentamicin+Tadalafil group received tadalafil (5mg/kg, P.O) for 12 days and on days 6-12, they received gentamicin (100mg/kg,i.p) one hour after oral administration of tadalafil. Body weight and kidney weight were investigated. Urine volume as well as urinary albumin, creatinine, creatinine clearance and albumin /creatinine ratio (ACR) performed. The results of the present study showed that GNT decreased creatinine clearance and increased the serum levels of renal function parameters. GNT caused a significant increase in renal cortex MDA, NO and urine levels of KIM-1, while it decreased CAT and SOD activities. Gentamicin administration resulted in increased immunohistochemical expression of iNOS enzyme while decreasing eNOS expression. Renal corpuscles and tubules also showed histological and ultrastructural changes. Pretreatment with tadalafil, on the other hand, reversed the effects of GNT administration. In conclusion , findings of the present study indicate that tadalafil reduces GNT-induced kidney damage by inhibition of inflammation, oxidative stress, and apoptosis.

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他达拉非对庆大霉素所致大鼠肾毒性的影响

背景:庆大霉素(GNT)是一种高效氨基糖苷类抗生素，通常用于治疗危及生命的细菌感染。目的:本研究的目的是确定他达拉非是否可以预防gnt引起的肾毒性。方法:选用雄性白化病大鼠24只，随机分为4组，每组6只。对照组连续12天灌胃蒸馏水(5ml/kg, P.O)，第6-12天灌胃生理盐水(5ml/kg,i.p)，灌胃蒸馏水后1 h。他达拉非组患者给予他达拉非(5mg/kg, P.O)治疗12 d，第6-12天口服他达拉非后1 h，每日给予生理盐水(5ml/kg,i.p)。庆大霉素组给予蒸馏水(5ml/kg, P.O)，第6-12天，在蒸馏水口服1 h后给予庆大霉素(011mg/kg,i.p)。庆大霉素+他达拉非组给予他达拉非(5mg/kg, P.O)治疗12 d，第6-12天，在口服他达拉非1 h后给予庆大霉素(100mg/kg,i.p)治疗。测定体重和肾脏重量。检查尿量、尿白蛋白、肌酐、肌酐清除率和白蛋白/肌酐比值(ACR)。本研究结果表明，GNT降低肌酐清除率，提高血清肾功能参数水平。GNT显著升高肾皮质MDA、NO和尿中KIM-1水平，降低CAT和SOD活性。庆大霉素引起iNOS酶免疫组化表达升高，eNOS表达降低。肾小体和肾小管也出现组织学和超微结构改变。另一方面，他达拉非预处理可以逆转GNT给药的效果。总之，本研究结果表明，他达拉非通过抑制炎症、氧化应激和细胞凋亡来减轻gnt诱导的肾损伤。

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Egyptian Journal of Medical Research

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