| Literature DB >> 28867614 |
Vitul Jain1, Manickam Yogavel1, Haruhisa Kikuchi2, Yoshiteru Oshima2, Norimitsu Hariguchi3, Makoto Matsumoto4, Preeti Goel1, Bastien Touquet5, Rajiv S Jumani6, Fabienne Tacchini-Cottier7, Karl Harlos8, Christopher D Huston6, Mohamed-Ali Hakimi5, Amit Sharma9.
Abstract
Developing anti-parasitic lead compounds that act on key vulnerabilities are necessary for new anti-infectives. Malaria, leishmaniasis, toxoplasmosis, cryptosporidiosis and coccidiosis together kill >500,000 humans annually. Their causative parasites Plasmodium, Leishmania, Toxoplasma, Cryptosporidium and Eimeria display high conservation in many housekeeping genes, suggesting that these parasites can be attacked by targeting invariant essential proteins. Here, we describe selective and potent inhibition of prolyl-tRNA synthetases (PRSs) from the above parasites using a series of quinazolinone-scaffold compounds. Our PRS-drug co-crystal structures reveal remarkable active site plasticity that accommodates diversely substituted compounds, an enzymatic feature that can be leveraged for refining drug-like properties of quinazolinones on a per parasite basis. A compound we termed In-5 exhibited a unique double conformation, enhanced drug-like properties, and cleared malaria in mice. It thus represents a new lead for optimization. Collectively, our data offer insights into the structure-guided optimization of quinazolinone-based compounds for drug development against multiple human eukaryotic pathogens.Entities:
Keywords: X-ray crystallography; coccidiosis; cryptosporidiosis; drug discovery; leishmaniasis; malaria; prolyl-tRNA synthetase; toxoplasmosis
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Year: 2017 PMID: 28867614 DOI: 10.1016/j.str.2017.07.015
Source DB: PubMed Journal: Structure ISSN: 0969-2126 Impact factor: 5.006