Bile acid synthesis impedes tumor-specific T cell responses during liver cancer [RNA-seq1]

The tumor's metabolic landscape significantly influences anti-tumor immunity, but it remains unclear how metabolic pathways commonly active in the organ of tumor-origin influence immunosurveillance. This study focused on the liver and identified accumulation of primary conjugated and secondary bile acids (BAs) as metabolic features associated with hepatocellular carcinoma and liver cancer models. Inhibiting conjugated BA synthesis through BAAT-deletion in hepatocytes enhanced tumor-specific T cell responses, reduced growth, and sensitized tumors to immune checkpoint blockade. BAs regulated CD8+ T cells differently; primary BAs like TCDCA induced oxidative stress and secondary BAs like LCA impaired T cell function through ER stress, which was countered by UDCA. Indeed, dietary UDCA provision suppressed tumor progression. These findings demonstrate how manipulating organ-specific metabolites affects antitumor immunity and modifying BA synthesis or dietary intake could enhance immunotherapy in liver cancer. To investigate the effect of bile acid treatment on T Cell gene expression. Gene expression profiling analysis using data obtained from RNA-seq of T Cells treated with different bile acids.in vitro activated CD8+ T cells were exposed with different bile acids for 24 hours following with RNA was isolated using Qiagen RNA isoaltion kit.