Anthraquinone derivatives as ADP-competitive inhibitors of liver pyruvate kinase.
Nain-Perez, A., Foller Fuchtbauer, A., Haversen, L., Lulla, A., Gao, C., Matic, J., Monjas, L., Rodriguez, A., Brear, P., Kim, W., Hyvonen, M., Boren, J., Mardinoglu, A., Uhlen, M., Grotli, M.(2022) Eur J Med Chem 234: 114270-114270
- PubMed: 35290845 
- DOI: https://doi.org/10.1016/j.ejmech.2022.114270
- Primary Citation of Related Structures:  
5SC8, 5SC9, 5SCA, 5SCB, 5SCC, 5SCD, 5SCE, 5SCF, 5SCG, 5SCH, 5SCI, 5SCJ, 5SCK, 5SCL, 5SDT, 7QDN, 7QZU - PubMed Abstract: 
Liver pyruvate kinase (PKL) is a major regulator of metabolic flux and ATP production during liver cell glycolysis and is considered a potential drug target for the treatment of non-alcoholic fatty liver disease (NAFLD). In this study, we report the first ADP-competitive PKL inhibitors and identify several starting points for the further optimization of these inhibitors. Modeling and structural biology guided the optimization of a PKL-specific anthraquinone-based compound. A structure-activity relationship study of 47 novel synthetic derivatives revealed PKL inhibitors with half-maximal inhibitory concentration (IC 50 ) values in the 200?nM range. Despite the difficulty involved in studying a binding site as exposed as the ADP site, these derivatives feature expanded structural diversity and chemical spaces that may be used to improve their inhibitory activities against PKL. The obtained results expand the knowledge of the structural requirements for interactions with the ADP-binding site of PKL.
Organizational Affiliation: 
Department of Chemistry and Molecular Biology, University of Gothenburg, SE-412 96, Gothenburg, Sweden.