Galectin-12 modulates Kupffer cell polarization to alter the progression of nonalcoholic fatty liver disease

Abstract: Non-alcoholic fatty liver disease (NAFLD) is caused by an imbalance in lipid metabolism and immune response to pose a risk factor for liver fibrosis. Recent evidence indicates that M2 macrophages secrete transforming growth factor (TGF)-β1, which contributes to liver fibrosis. Galectin-12 (Gal12) has been demonstrated to regulate lipid metabolism and macrophage polarization. The purpose of this study is to investigate the role of Gal12 in the development of NAFLD and fibrosis. Liver tissue from wild-type C57BL… Show more

“…The elevated levels of LEPR and SOCS3 mRNA in both the OAT and liver associated with IR indicate a post-receptor mechanism with a predominance of negative feedback in peripheral tissue. Our data align with the differences between MASLD and MASH biopsies in the presence of SOCS3 [130], as well as with studies showing that SOCS3 inhibition prevents M1 polarization of Kupffer cells and steatotic progression to inflammation [131]. This demonstrates that comparable events occur in the liver and CNS [132,133].…”

Evidence That Peripheral Leptin Resistance in Omental Adipose Tissue and Liver Correlates with MASLD in Humans

“…The elevated levels of LEPR and SOCS3 mRNA in both the OAT and liver associated with IR indicate a post-receptor mechanism with a predominance of negative feedback in peripheral tissue. Our data align with the differences between MASLD and MASH biopsies in the presence of SOCS3 [130], as well as with studies showing that SOCS3 inhibition prevents M1 polarization of Kupffer cells and steatotic progression to inflammation [131]. This demonstrates that comparable events occur in the liver and CNS [132,133].…”

Evidence That Peripheral Leptin Resistance in Omental Adipose Tissue and Liver Correlates with MASLD in Humans