Bicyclol attenuates high fat diet-induced non-alcoholic fatty liver disease/non-alcoholic steatohepatitis through modulating multiple pathways in mice

Wu, Jingyi; Jia, Shu Fang; Xu, Benghong; Yao, Xiaokun; Shao, Jingping; Yao, Jianzuo; Cen, Danwei; Yao, Xiaomin

doi:10.3389/fphar.2023.1157200

Cited by 2 publications

(1 citation statement)

References 38 publications

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“…In vitro studies confirm that GSTA1 has the highest catalytic activity among human GSTs for the GSH conjugation of toxic substances and lipid peroxidation products [39]. The expression of GSTA1 was decreased in mouse models of MASLD induced by HFD-feeding [40], in mouse and patient livers [41], and in HepG2 cells treated with proinflammatory cytokines [42]. Consistent with these results, we observed decreased GSTA1 expression in the livers of MASLD mice and patients and in hepatocytes induced by free fatty acids in vitro.…”

Section: Discussionmentioning

confidence: 75%

Upregulation of Hepatic Glutathione S-Transferase Alpha 1 Ameliorates Metabolic Dysfunction-Associated Steatosis by Degrading Fatty Acid Binding Protein 1

Jiang,

Li,

Tang

et al. 2024

IJMS

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Metabolic dysfunction-associated steatotic liver disease (MASLD) is the most common metabolic disease of the liver, characterized by hepatic steatosis in more than 5% of hepatocytes. However, despite the recent approval of the first drug, resmetirom, for the management of metabolic dysfunction-associated steatohepatitis, decades of target exploration and hundreds of clinical trials have failed, highlighting the urgent need to find new druggable targets for the discovery of innovative drug candidates against MASLD. Here, we found that glutathione S-transferase alpha 1 (GSTA1) expression was negatively associated with lipid droplet accumulation in vitro and in vivo. Overexpression of GSTA1 significantly attenuated oleic acid-induced steatosis in hepatocytes or high-fat diet-induced steatosis in the mouse liver. The hepatoprotective and anti-inflammatory drug bicyclol also attenuated steatosis by upregulating GSTA1 expression. A detailed mechanism showed that GSTA1 directly interacts with fatty acid binding protein 1 (FABP1) and facilitates the degradation of FABP1, thereby inhibiting intracellular triglyceride synthesis by impeding the uptake and transportation of free fatty acids. Conclusion: GSTA1 may be a good target for the discovery of innovative drug candidates as GSTA1 stabilizers or enhancers against MASLD.

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