Could Hesperidin and Iron chelator be a new Therapeutic approach in Gentamicin induced Acute Kidney Injury in Rats?

Physiology Department, Benha Faculty of Medicine, Benha University, Qalubiya, Egypt

^*Corresponding Author

Marwa H. Muhammad

Physiology Department

Benha Faculty of Medicine

Benha University

Qalubiya

Egypt

Cell no.002 01009655692

Email: drmarwa.hassan@yahoo.com

Abstract

Kidney function is maintaining of homeostasis and toxins elimination. Thus, it is susceptible to acute damage by xenobiotics. Drug-induced nephrotoxicity is becoming a principal etiology for acute kidney injury (AKI). The present study was designed to investigate the protective effect of iron chelator, desferroxamin (DFO), and hesperidin (HES) on gentamicin (GM) induced AKI in rats and elucidating the potential mechanisms. Group I: control, group II: GM (100mg/kg/d. i.p.) for 7days, group III: HES (200 mg/ kg) two days before and 7 days concomitantly with GM, group IV: DFO (100 mg/kg/d. i.p.) co-administrated with GM and group V: GM + combined treatment by DFO and HES. Serum urea, creatinine, KIM1, TNF-α and IL-6, renal MDA and HO1 concentration, immunohistochemical expression of caspase 3 and histopathology of kidney were evaluated. GM induced significant increase in all parameters excluding renal HO1 level which is significantly decreased (p<0.05). Histopathological examinations revealed acute tubular necrosis, hemorrhage and interstitial nephritis. These results were significantly reversed upon either therapy by DFO or HES with more protection by combined treatment. These findings suggest that the Reno-protective mechanisms of HES and DFO including antioxidant, anti-inflammatory and anti-apoptotic effects. They are a good therapeutic approach for treating gentamicin nephrotoxicity.

Keywords: Desferroxamin, Hesperidin, Acute kidney injury, Gentamicin

Download the full article (PDF)