4.7 Article

Oral Nigella sativa oil administration alleviates arsenic-induced redox imbalance, DNA damage, and metabolic and histological alterations in rat liver

Journal

ENVIRONMENTAL SCIENCE AND POLLUTION RESEARCH
Volume 28, Issue 30, Pages 41464-41478

Publisher

SPRINGER HEIDELBERG
DOI: 10.1007/s11356-021-13493-6

Keywords

Sodium arsenate; Nigella sativa oil; Hepatotoxicity; Oxidative stress; Carbohydrate metabolism

Funding

  1. Department of Biochemistry from the UGC-SAP-DRS III, DST-FIST program
  2. Department of Biochemistry from the UGC-SAP-DRS III, DBT-PURSE program
  3. DBT (Department of Biotechnology), Government of India

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Arsenic is a potent hepatotoxin, while studies have shown that Nigella sativa oil has a protective effect on acute liver injury and can improve liver function. Experimental findings suggest that Nigella sativa oil can alleviate liver damage caused by arsenic, and improve the antioxidant and metabolic status of the liver.
Arsenic, an omnipresent environmental contaminant, is regarded as a potent hepatotoxin. Nigella sativa oil (NSO) consumption has been shown to improve hepatic functions in various in vivo models of acute hepatic injury. The present study evaluates the protective efficacy of NSO against sodium arsenate (As)-induced deleterious alterations in the liver. Male Wistar rats were divided into four groups, namely, control, As, NSO, and AsNSO. After pre-treating rats in AsNSO and NSO groups with NSO (2 mL/kg bwt, orally) for 14 days, NSO treatment was further extended for 30 days, with and without As treatment (5 mg/kg bwt, orally), respectively. As induced an upsurge in serum ALT and AST activities indicating liver injury, as also confirmed by the histopathological findings. As caused significant alterations in the activities of membrane marker enzymes and carbohydrate metabolic enzymes, and in the vital components of antioxidant defense system. Marked DNA damage and hepatic arsenic accumulation were also observed in As-treated rats. Oral NSO administration ameliorated these deleterious alterations and improved overall hepatic antioxidant and metabolic status in As-treated rats. Prevention of oxidative damage could be the underlying mechanism of NSO-mediated protective effects. The results suggest that NSO could be a useful dietary supplement in the management of arsenic hepatotoxicity.

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