Abstract

Hepatic Sodium Taurocholate cotransporter polypeptide (NTCP1) captures approximately 80% of the conjugated bile acids that come from the enterohepatic circulation. Transcriptionally, NTCP1 expression is activated by an RAR/RXR heterodimer, which is repressed by SHP when intracellular bile acids are high. In addition, NTCP1 activity is post-translational modulated by phosphorylation. However, whether NTCP1 could be regulated by acetylation is unknown. A bioinformatic analysis for the mouse NTCP1 protein sequence showed potential lysine acetylation sites. Thus, we evaluated taurocholate uptake in hepatocytes incubated with NAM, which induced a two-fold increase in the content of acetylated proteins. Interestingly, taurocholate uptake was reduced by 50% in hepatocytes incubated with NAM. These results demonstrate that acetylation mediates taurocholate uptake in hepatocytes possibly through modulation of NTCP1 activity.

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