Blocking TRIM47-mediated HNF4 degradation suppresses hepatocellular carcinoma progression.

Previous studies have highlighted the downregulation of hepatocyte nuclear factor 4alpha (HNF4) as a critical event in the pathogenesis of HCC. However, the mechanism of its degradation in HCC remains unclear. Tripartite motif 47 (TRIM47), a typical E3 ubiquitin ligase of the TRIM family, has been implicated in various tumors, yet its specific role in HCC progression is not fully elucidated. In this study, HNF4 was identified as a potential target of TRIM47 by using co-immunoprecipitation (Co-IP) combined with mass spectrometry analysis. TRIM47 facilitates the degradation of HNF4 by mediating K48-linked ubiquitination at lysine 470. Abrogation of HNF4 ubiquitination attenuated the promoting effect of TRIM47 on HCC malignancy. Molecular docking studies and Co-IP experiments revealed that K342, W349, and E353 of HNF4, along with K534 and K600 of TRIM47, are crucial for their interaction. A small molecule, CZ-2401, was selected as a potent inhibitor of the TRIM47-HNF4 interaction through virtual screening and pharmacological activity validation. CZ-2401 effectively stabilizes HNF4 protein in HCC cells and ameliorates TRIM47-driven HCC progression Taken together, our research elucidates that targeting TRIM47-HNF4 interaction is a potential therapeutic strategy for HCC, and identifies CZ-2401 as a potent inhibitor of HNF4 degradation and a promising candidate for HCC therapy.