Hesperidin mitigates Doxorubicin-induced hepatic toxicity in rats, targeting JAK-STAT signaling pathway

Khodir, Suzan A; Nagy, Alaa; Abd El-aziz, Noha; Mohamed, Amira; hussein, samar; Elgheriany, walaa; Abd-Elhamid, tarek; Elnady, Maha; zayed, mohamed

doi:10.21608/mjfmct.2024.330487.1086

	Hesperidin mitigates Doxorubicin-induced hepatic toxicity in rats, targeting JAK-STAT signaling pathway
Mansoura Journal of Forensic Medicine and Clinical Toxicology
Volume 33, Issue 1, January 2025, Page 33-43 PDF (1.08 MB)
Document Type: Original Article
DOI: 10.21608/mjfmct.2024.330487.1086
View on SCiNiTO
Authors
Suzan A Khodir ¹; Alaa Nagy²; Noha Abd El-aziz³; Amira Mohamed⁴; samar hussein⁵; walaa Elgheriany⁶; tarek Abd-Elhamid⁷; Maha Elnady⁸; mohamed zayed⁹
¹physiology department, faculty of medicine, menoufia university
²Medical Biochemistry and Molecular Biology Department, Faculty of medicine, Menoufia University
³Anatomy and Embryology Department, Faculty of Medicine, Menoufia University
⁴Pharmacology Department, Faculty of medicine, Suez Canal University
⁵Medical Physiology Department, Faculty of Medicine, Suez Canal University
⁶Internal Medicine department Faculty of Medicine, Menoufia University, Shebin El-Kom, Menoufia, Egypt.
⁷Histology and Cell Biology, Faculty of Medicine, Assiut University Histology, Faculty of Medicine, Aqaba Medical Sciences University
⁸Forensic Medicine and Clinical Toxicology department, Faculty of Medicine, Menoufia University
⁹Medical Physiology Department, Faculty of Medicine, Menoufia University Medical physiology department, Faculty of medicine, king Abdulaziz University
Abstract
Even though doxorubicin (DOX) is an excellent cancer chemotherapy, its adverse impacts, including hepatotoxicity, restrict its clinical usefulness. The study's goal was to assess hesperidin's (HSP) hepatoprotective impact in rats exposed to DOX as well as any potential underlying mechanisms. Thirty male albino rats were split into three: DOX, DOX+HSP, and control (10/group). Serum liver enzymes, triglycerides (TG) and cholesterol, hepatic MDA, superoxide dismutase (SOD), serum TNF-α, IL-6, IL-10, liver-expressed JAK2, STAT3 genes, and organ index were assessed. There were additional evaluations of NF-kB and caspase-3 immunoreactions in the liver. The results revealed that hepatic SOD, IL-10, and liver index values all substantially declined in response to DOX-induced damage. But compared to the control group, there was a dramatic rise in the JAK2 and STAT3 genes, as well as hepatic MDA, TNF-α, and IL-6. There was also an increase in blood liver enzymes, serum cholesterol, and TG. In the liver, caspase-3 and NF-kB immunoreactions were also up-regulated. HSP dramatically improved DOX-induced changes in the liver. It can be concluded that, in addition to down-regulating the JAK2/STAT3 signaling cascade, HSP also employed antioxidant, anti-inflammatory, and anti-apoptotic mechanisms to mitigate the hepatotoxicity induced by DOX.
Keywords
Caspase3; DOX; JAK2; NF-kB; STAT3
Supplementary Files figure 1 liver.jpg WhatsApp Image 2025-02-22 at 11.01.32 AM.jpeg

Statistics Article View: 190 PDF Download: 96