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Carbon tetrachloride does not promote hepatic fibrosis in ob/ob mice via downregulation of lipocalin-2 proteinopen access
- Authors
- Shin, Hyun Joo; Kim, Kyung Eun; An, Hyeong Seok; Jeong, Eun Ae; Oh, Jiwon; Sun, Yundong; Park, Dong-Ju; Lee, Jaewoong; Yang, Jinsung; Roh, Gu Seob
- Issue Date
- Mar-2025
- Publisher
- Elsevier BV
- Keywords
- Carbon tetrachloride; Hepatic fibrosis; Lipocalin-2; Ob/ob mouse
- Citation
- Redox Biology, v.80
- Indexed
- SCIE
SCOPUS
- Journal Title
- Redox Biology
- Volume
- 80
- ISSN
- 2213-2317
- Abstract
- Although leptin-deficient ob/ob mice have been investigated to determine whether hepatic steatosis promotes susceptibility to hepatotoxic insults, carbon tetrachloride (CCl4)-induced hepatic fibrosis in ob/ob mice remains largely unknown. In this study, we evaluate the pathogenic mechanisms of hepatic fibrosis in CCl4-treated wild-type (WT) and ob/ob mice and analyze some parameters related to lipogenesis, inflammation, fibrosis, oxidative stress, apoptosis, and autophagy. CCl4 treatment attenuated liver weight and lipogenesis in ob/ob mice. Increased hepatic fibrosis-related proteins were reduced in CCl4-treated ob/ob mice compared with CCl4-treated WT mice. Specifically, the expression of lipocalin-2 (LCN2) was markedly reduced in CCl4-treated ob/ob mice versus CCl4-treated WT mice. Compared with CCl4-treated WT mice, CCl4-treated ob/ob mice had reduced expression of neutrophil-related inflammatory genes and proteins. Hepatic heme oxygenase-1 protein was reduced in CCl4-treated ob/ob mice compared with CCl4-treated WT mice. However, CCl4 did not promote hepatic apoptosis in ob/ob mice. Therefore, these findings highlight LCN2 as a key signaling factor in CCl4-induced hepatic fibrosis. © 2025 The Authors
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