| Literature DB >> 29578710 |
Sebastian Pomplun1, Claudia Sippel1, Andreas Hähle1,2, Donald Tay3, Kensuke Shima4, Alina Klages5, Can Murat Ünal5, Benedikt Rieß1, Hui Ting Toh3, Guido Hansen6, Ho Sup Yoon3, Andreas Bracher7, Peter Preiser3, Jan Rupp4, Michael Steinert4,8, Felix Hausch1,2.
Abstract
FK506-binding proteins (FKBPs) are evolutionarily conserved proteins that display peptidyl-prolyl isomerase activities and act as coreceptors for immunosuppressants. Microbial macrophage-infectivity-potentiator (Mip)-type FKBPs can enhance infectivity. However, developing druglike ligands for FKBPs or Mips has proven difficult, and many FKBPs and Mips still lack biologically useful ligands. To explore the scope and potential of C5-substituted [4.3.1]-aza-bicyclic sulfonamides as a broadly applicable class of FKBP inhibitors, we developed a new synthesis method for the bicyclic core scaffold and used it to prepare an FKBP- and Mip-focused library. This allowed us to perform a systematic structure-activity-relationship analysis across key human FKBPs and microbial Mips, yielding highly improved inhibitors for all the FKBPs studied. A cocrystal structure confirmed the molecular-binding mode of the core structure and explained the affinity gained as a result of the preferred substituents. The best FKBP and Mip ligands showed promising antimalarial, antileginonellal, and antichlamydial properties in cellular models of infectivity, suggesting that substituted [4.3.1]-aza-bicyclic sulfonamides could be a novel class of anti-infectives.Entities:
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Year: 2018 PMID: 29578710 DOI: 10.1021/acs.jmedchem.8b00137
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446