Cardioprotective and Hepatoprotective Potential of Silymarin in Paracetamol-Induced Oxidative Stress

Author:

Okiljević Bogdan1ORCID,Martić Nikola2ORCID,Govedarica Srđan34ORCID,Andrejić Višnjić Bojana5ORCID,Bosanac Milana5ORCID,Baljak Jovan4,Pavlić Branimir6ORCID,Milanović Isidora7,Rašković Aleksandar2

Affiliation:

1. Department of Cardiac Surgery, Dedinje Cardiovascular Institute, 11000 Belgrade, Serbia

2. Department of Pharmacology, Toxicology, and Clinical Pharmacology, Faculty of Medicine, University of Novi Sad, 21000 Novi Sad, Serbia

3. Clinic of Urology, Clinical Center of Vojvodina, 21000 Novi Sad, Serbia

4. Faculty of Medicine, University of Novi Sad, 21000 Novi Sad, Serbia

5. Department of Histology and Embryology, Faculty of Medicine, University of Novi Sad, 21000 Novi Sad, Serbia

6. Faculty of Technology, University of Novi Sad, 21000 Novi Sad, Serbia

7. Department of Pharmacology, Biochemistry, Pharmacy and Ecology, Academy for Applied Studies Belgrade, College of Health Sciences, 11080 Belgrade, Serbia

Abstract

Silymarin, derived from Silybum marianum, has been used in traditional medicine for various ailments. In this study, the cardioprotective and hepatoprotective effects of silymarin against paracetamol-induced oxidative stress were examined in 28 male Swiss Webster mice, divided into four groups and treated for 7 days (via the oral route) with (a) saline 1 mL/kg (control group), (b) saline 1 mL/kg + single dose of paracetamol 110 mg/kg on the 7th day; (c) silymarin 50 mg/kg; and (d) silymarin 50 mg/kg + single dose of paracetamol 110 mg/kg on the 7th day. In vitro and in vivo antioxidant activity together with liver enzyme activity were evaluated. Histopathological and immunohistochemical assessment was performed. Silymarin mitigated paracetamol-induced liver injury by reducing oxidative stress markers such as lipid peroxidation and restoring antioxidant enzyme activity. Silymarin treatment resulted in a significant decrease in liver enzyme levels. Reduced necrosis and inflammatory infiltrate in liver tissues of silymarin-treated groups were detected as well. Immunohistochemical analysis demonstrated reduced expression of inflammatory markers (COX2, iNOS) and oxidative stress marker (SOD2) in the liver tissues of the silymarin-treated groups. Similar trends were observed in cardiac tissue. These results suggest that silymarin exerts potent hepatoprotective and cardioprotective effects against paracetamol-induced oxidative stress, making it a promising therapeutic agent for liver and heart diseases associated with oxidative damage.

Funder

Pokrajinski Sekretarijat za Nauku i Tehnološki Razvoj

Publisher

MDPI AG

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