Identification and characterization of a new potent inhibitor targeting CtBP1/BARS in melanoma cells

Filograna, Angela; De Tito, Stefano; Monte, Matteo Lo; Oliva, Rosario; Bruzzese, Francesca; Roca, Maria Serena; Zannetti, Antonella; Greco, Adelaide; Spano, Daniela; Ayala, Inmaculada; Liberti, Assunta; Petraccone, Luigi; Dathan, Nina; Catara, Giuliana; Schembri, Laura; Colanzi, Antonino; Budillon, Alfredo; Beccari, Andrea Rosario; Del Vecchio, Pompea; Luini, Alberto; Corda, Daniela; Valente, Carmen

doi:10.1186/s13046-024-03044-5

Background: The C-terminal-binding protein 1/brefeldin A ADP-ribosylation substrate (CtBP1/BARS) acts both as an oncogenic transcriptional co-repressor and as a fission inducing protein required for membrane trafficking and Golgi complex partitioning during mitosis, hence for mitotic entry. CtBP1/BARS overexpression, in multiple cancers, has pro-tumorigenic functions regulating gene networks associated with "cancer hallmarks" and malignant behavior including: increased cell survival, proliferation, migration/invasion, epithelial-mesenchymal transition (EMT). Structurally, CtBP1/BARS belongs to the hydroxyacid-dehydrogenase family and possesses a NAD(H)-binding Rossmann fold, which, depending on ligands bound, controls the oligomerization of CtBP1/BARS and, in turn, its cellular functions. Here, we proposed to target the CtBP1/BARS Rossmann fold with small molecules as selective inhibitors of mitotic entry and pro-tumoral transcriptional activities. Methods: Structured-based screening of drug databases at different development stages was applied to discover novel ligands targeting the Rossmann fold. Among these identified ligands, N-(3,4-dichlorophenyl)-4-{[(4-nitrophenyl)carbamoyl]amino}benzenesulfonamide, called Comp.11, was selected for further analysis. Fluorescence spectroscopy, isothermal calorimetry, computational modelling and site-directed mutagenesis were employed to define the binding of Comp.11 to the Rossmann fold. Effects of Comp.11 on the oligomerization state, protein partners binding and pro-tumoral activities were evaluated by size-exclusion chromatography, pull-down, membrane transport and mitotic entry assays, Flow cytometry, quantitative real-time PCR, motility/invasion, and colony assays in A375MM and B16F10 melanoma cell lines. Effects of Comp.11 on tumor growth in vivo were analyzed in mouse tumor model. Results: We identify Comp.11 as a new, potent and selective inhibitor of CtBP1/BARS (but not CtBP2). Comp.11 directly binds to the CtBP1/BARS Rossmann fold affecting the oligomerization state of the protein (unlike other known CtBPs inhibitors), which, in turn, hinders interactions with relevant partners, resulting in the inhibition of both CtBP1/BARS cellular functions: i) membrane fission, with block of mitotic entry and cellular secretion; and ii) transcriptional pro-tumoral effects with significantly hampered proliferation, EMT, migration/invasion, and colony-forming capabilities. The combination of these effects impairs melanoma tumor growth in mouse models. CONCLUSIONS: This study identifies a potent and selective inhibitor of CtBP1/BARS active in cellular and melanoma animal models revealing new opportunities to study the role of CtBP1/BARS in tumor biology and to develop novel melanoma treatments.

Identification and characterization of a new potent inhibitor targeting CtBP1/BARS in melanoma cells / Filograna, Angela; De Tito, Stefano; Monte, Matteo Lo; Oliva, Rosario; Bruzzese, Francesca; Roca, Maria Serena; Zannetti, Antonella; Greco, Adelaide; Spano, Daniela; Ayala, Inmaculada; Liberti, Assunta; Petraccone, Luigi; Dathan, Nina; Catara, Giuliana; Schembri, Laura; Colanzi, Antonino; Budillon, Alfredo; Beccari, Andrea Rosario; Del Vecchio, Pompea; Luini, Alberto; Corda, Daniela; Valente, Carmen. - In: JOURNAL OF EXPERIMENTAL & CLINICAL CANCER RESEARCH. - ISSN 1756-9966. - 43:(2024). [10.1186/s13046-024-03044-5]