L-Carnitine protects kidney against ischemia reperfusion injury via suppression of expression of tubular kidney injury molecule (Kim-1) and Wnt proteins (Beta- Catenin)
Adel, M., rami, M., shaheen, D., Monir, R., basheir, M., nabawy, A., eladl, A. (2020). L-Carnitine protects kidney against ischemia reperfusion injury via suppression of expression of tubular kidney injury molecule (Kim-1) and Wnt proteins (Beta- Catenin). EKB Journal Management System, 40(1), 32-45. doi: 10.21608/besps.2019.14073.1023
Mohamed Adel; mohamed rami; dalia shaheen; Rehan Monir; mamdouh basheir; ahmed nabawy; ahmed eladl. "L-Carnitine protects kidney against ischemia reperfusion injury via suppression of expression of tubular kidney injury molecule (Kim-1) and Wnt proteins (Beta- Catenin)". EKB Journal Management System, 40, 1, 2020, 32-45. doi: 10.21608/besps.2019.14073.1023
Adel, M., rami, M., shaheen, D., Monir, R., basheir, M., nabawy, A., eladl, A. (2020). 'L-Carnitine protects kidney against ischemia reperfusion injury via suppression of expression of tubular kidney injury molecule (Kim-1) and Wnt proteins (Beta- Catenin)', EKB Journal Management System, 40(1), pp. 32-45. doi: 10.21608/besps.2019.14073.1023
Adel, M., rami, M., shaheen, D., Monir, R., basheir, M., nabawy, A., eladl, A. L-Carnitine protects kidney against ischemia reperfusion injury via suppression of expression of tubular kidney injury molecule (Kim-1) and Wnt proteins (Beta- Catenin). EKB Journal Management System, 2020; 40(1): 32-45. doi: 10.21608/besps.2019.14073.1023

L-Carnitine protects kidney against ischemia reperfusion injury via suppression of expression of tubular kidney injury molecule (Kim-1) and Wnt proteins (Beta- Catenin)

Bulletin of Egyptian Society for Physiological Sciences
Article 3, Volume 40, Issue 1, January 2020, Page 32-45  XML PDF (631.21 K)
Document Type: Original Article
DOI: 10.21608/besps.2019.14073.1023
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Authors
Mohamed Adel email 1; mohamed rami1; dalia shaheen2; Rehan Monir3; mamdouh basheir4; ahmed nabawy4; ahmed eladl5
1Department of Medical Physiology, Faculty of Medicine, Mansoura University, Egypt
2Department of Biochemistry, Faculty of Medicine, Mansoura University, Egypt
3Department of Biochemistry, Faculty of Medicine, Mansoura University, Egypt faculty of medicine, king khalid university
4Department of Anatomy, Faculty of Medicine, Mansoura University, Egypt
5Department of Pathology, Faculty of Medicine, Mansoura University, Egypt
Abstract
L-Carnitine is a unique nutritional supplement for athletes that has been recently studied as a potential treatment for certain renal disorders. However, its efficacy in renal ischemia reperfusion injuries has not been investigated. Rats were randomly assigned to one of five groups (n = 6/group):1, Control negative: received saline, 2,control positive I/R, rats received Sal and ischemia reperfusion at the end of fourth week and 3, L-Car +I/R group: same as Sal and ischemia reperfusion, but rats received L-Car (100 mg∕ kg) intraperitoneally daily for four weeks, 4, metformin +I/R group: same as Sal and ischemia reperfusion, but rats received oral metformin (300 mg/kg/day) daily for four weeks. 5, metformin +I/R group +L-Car: same as group 3, but rats received oral metformin (300 mg/kg/day) daily for four weeks. IR induced a significant increase in serum creatinine, serum K⁺ and serum KIM-1 peaked at 24 hours after I/R. KIM-1 and β -catenin expression is upregulated 168 hours after I/R. L-Car administration led to a significant decrease in serum creatinine in proportional to I/R group, serum K⁺ in proportional to I/R group, and a significant decrease in serum KIM-1 and Kim-1 expression. L-Car administration attenuated I/R-induced increase in oxidative stress marker MDA and increased antioxidant GSH activity. Moreover, the inducer of autophagy (Metformin) led to a significant decrease in serum creatinine, serum K⁺ and a significant decrease in serum Kim-1 and Kim-1 expression in renal tissue. Overall, our results suggest a potential therapeutic role of L-Car and metformin in I/R
Keywords
L-carnitine; Beta- Catenin; Kim-1
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