Gut Microbiota and HMGB1/NLRP3/GSDMD Inflammasome-Dependent Pyroptosis: Mechanisms by Physcion Ameliorates Alcoholic Liver Fibrosis

Alcoholic liver \ufb01brosis (ALF) developed from long-term excessive alcohol consumption, which causes in\ufb02ammatory reactions, lipid accumulation and cirrhosis. An imbalance in gut microbiota is a crucial driving factor for liver \ufb01brosis through the gut-liver axis. This study aimed to explore the effect of physcion on ALF associated with HMGB1/NLRP3 pathways and gut microbiota. C57BL/6 mice were used to establish animal model of ALF, LX-2 cells were used to establish alcohol-activated cell model, the intestinal contents of the mice were collected and analyzed by 16S rRNA sequencing. Physcion effectively ameliorated ALF-induced in\ufb02ammation, collagen deposition, lipid accumulation by SirT1, AMPK phosphorylation and SREBP1 expression. Moreover, pyroptosis-related proteins (Caspase-1, IL-1\u03b2, GSDMD) were signi\ufb01cantly reduced after physcion treatment. Interestingly, the diversity of intestinal bacteria and the abundance in physcion treatment mice was signi\ufb01cantly higher, while the abundance of harmful bacteria was signi\ufb01cantly lower than that in ALF mice. Importantly, it was found that physcion inhibit HMGB1/NLRP3 pathways both in vivo and in vitro, and suppress accumulation of extracellular matrix by inhibiting Collagen-I and \u03b1SMA to \ufb01nally reverse hepatic stellate cells activation. Continuous administration of HMGB1 and NLRP3 inhibitors showed hepato-protection in alcohol-activated LX-2 model. siRNA-mediated knock-down in LX-2 cells of HMGB1 signi\ufb01cantly impaired physcion-mediated protection. Regulation of the HMGB1/NLRP3 pathway recovered hepatic injury and further contributed to physcion\u2019s bene\ufb01cial effects. Taken together, the results reveal that physcion diminishes HMGB1/NLRP3 in\ufb02ammasome/pyroptosis and that this diminishment is hepatoprotective against ALF.