Integrated metabolomics and network pharmacology revealing the mechanism of arsenic-induced hepatotoxicity in mice

Yazhi Wang; Weina Cheng; Xiaoning Wang; Tianmu He; Jingxian Liu; Shuangshuang Chen; Jianyong Zhang

doi:10.1016/j.fct.2023.113913

Integrated metabolomics and network pharmacology revealing the mechanism of arsenic-induced hepatotoxicity in mice

Food Chem Toxicol. 2023 Aug:178:113913. doi: 10.1016/j.fct.2023.113913. Epub 2023 Jun 20.

Authors

Yazhi Wang¹, Weina Cheng¹, Xiaoning Wang¹, Tianmu He², Jingxian Liu³, Shuangshuang Chen¹, Jianyong Zhang⁴

Affiliations

¹ Department of Pharmaceutical Analysis, School of Pharmacy, Zunyi Medical University, Zunyi, 563000, China.
² School of Basic Medical Sciences, Zunyi Medical University, Zunyi, 563000, China; School of Basic Medical Sciences, Guizhou Medical University, Guiyang, 550025, China.
³ School of Basic Medical Sciences, Zunyi Medical University, Zunyi, 563000, China.
⁴ Department of Pharmaceutical Analysis, School of Pharmacy, Zunyi Medical University, Zunyi, 563000, China. Electronic address: zhangjianyong2006@126.com.

PMID: 37348806
DOI: 10.1016/j.fct.2023.113913

Abstract

Endemic arsenic (As) poisoning is a severe biogeochemical disease that endangers human health. Epidemiological investigations and animal experiments have confirmed the damaging effects of As on the liver, but there is an urgent need to investigate the underlying mechanisms. This study adopted a metabolomic approach using UHPLC-QE/MS to identify the different metabolites and metabolic mechanisms associated with As-induced hepatotoxicity in mice. A network pharmacology approach was applied to predict the potential target of As-induced hepatotoxicity. The predicted targets of differential metabolites were subjected to a deep matching for elucidating the integration mechanisms. The results demonstrate that the levels of ALT and AST in plasma significantly increased in mice after As exposure. In addition, the liver tissue showed disorganized liver lobules, lax cytoplasm and inflammatory cell infiltration. Metabolomic analysis revealed that As exposure caused disturbance to 40 and 75 potential differential metabolites in plasma and liver, respectively. Further investigation led to discovering five vital metabolic pathways, including phenylalanine, tyrosine, and tryptophan biosynthesis and nicotinate and nicotinamide metabolism pathways. These pathways may responded to As-induced hepatotoxicity primarily through lipid metabolism, apoptosis, and deoxyribonucleic acid damage. The network pharmacology suggested that As could induce hepatotoxicity in mice by acting on targets including Hsp90aa1, Akt2, Egfr, and Tnf, which regulate PI3K Akt, HIF-1, MAPK, and TNF signaling pathways. Finally, the integrated metabolomics and network pharmacology revealed eight key targets associated with As-induced hepatoxicity, namely DNMT1, MAOB, PARP1, MAOA, EPHX2, ANPEP, XDH, and ADA. The results also suggest that nicotinic acid and nicotinamide metabolisms may be involved in As-induced hepatotoxicity. This research identified the metabolites, targets, and mechanisms of As-induced hepatotoxicity, offering meaningful insights and establishing the groundwork for developing antidotes for widespread As poisoning.

Keywords: Arsenic; Hepatotoxicity; Mechanism; Metabolic pathways; Metabolomics; Network pharmacology.

MeSH terms

Animals
Arsenic* / toxicity
Chemical and Drug Induced Liver Injury*
Drugs, Chinese Herbal*
Humans
Metabolomics / methods
Mice
Network Pharmacology
Niacinamide
Phosphatidylinositol 3-Kinases

Substances

Arsenic
Phosphatidylinositol 3-Kinases
Niacinamide
Drugs, Chinese Herbal