| Literature DB >> 35675511 |
Ina Pöhner1,2, Antonio Quotadamo3,4, Joanna Panecka-Hofman1,5, Rosaria Luciani6, Matteo Santucci6, Pasquale Linciano6, Giacomo Landi7, Flavio Di Pisa7, Lucia Dello Iacono7, Cecilia Pozzi7, Stefano Mangani7, Sheraz Gul8, Gesa Witt8, Bernhard Ellinger8, Maria Kuzikov8, Nuno Santarem9, Anabela Cordeiro-da-Silva9,10, Maria P Costi6, Alberto Venturelli3,6, Rebecca C Wade1,2,11,12.
Abstract
The optimization of compounds with multiple targets is a difficult multidimensional problem in the drug discovery cycle. Here, we present a systematic, multidisciplinary approach to the development of selective antiparasitic compounds. Computational fragment-based design of novel pteridine derivatives along with iterations of crystallographic structure determination allowed for the derivation of a structure-activity relationship for multitarget inhibition. The approach yielded compounds showing apparent picomolar inhibition of T. brucei pteridine reductase 1 (PTR1), nanomolar inhibition of L. major PTR1, and selective submicromolar inhibition of parasite dihydrofolate reductase (DHFR) versus human DHFR. Moreover, by combining design for polypharmacology with a property-based on-parasite optimization, we found three compounds that exhibited micromolar EC50 values against T. brucei brucei while retaining their target inhibition. Our results provide a basis for the further development of pteridine-based compounds, and we expect our multitarget approach to be generally applicable to the design and optimization of anti-infective agents.Entities:
Mesh:
Substances:
Year: 2022 PMID: 35675511 PMCID: PMC9289884 DOI: 10.1021/acs.jmedchem.2c00232
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 8.039