Litcius/Paper detail

Re-emerging Aspartic Protease Targets: Examining <i>Cryptococcus neoformans</i> Major Aspartyl Peptidase 1 as a Target for Antifungal Drug Discovery

Robin Kryštůfek, Pavel Šácha, Jana Starková, J. Brynda, Martin Hradílek, Eva Tloušťová, Justyna Grzymska, Wioletta Rut, Michael J. Boucher, Marcin Drąg, Pavel Majer, Miroslav Hájek, Pavlína Řezáčová, Hiten D. Madhani, Charles S. Craik, Jan Konvalinka

2021Journal of Medicinal Chemistry28 citationsDOIOpen Access PDF

Abstract

Cryptococcosis is an invasive infection that accounts for 15% of AIDS-related fatalities. Still, treating cryptococcosis remains a significant challenge due to the poor availability of effective antifungal therapies and emergence of drug resistance. Interestingly, protease inhibitor components of antiretroviral therapy regimens have shown some clinical benefits in these opportunistic infections. We investigated Major aspartyl peptidase 1 (May1), a secreted Cryptococcus neoformans protease, as a possible target for the development of drugs that act against both fungal and retroviral aspartyl proteases. Here, we describe the biochemical characterization of May1, present its high-resolution X-ray structure, and provide its substrate specificity analysis. Through combinatorial screening of 11,520 compounds, we identified a potent inhibitor of May1 and HIV protease. This dual-specificity inhibitor exhibits antifungal activity in yeast culture, low cytotoxicity, and low off-target activity against host proteases and could thus serve as a lead compound for further development of May1 and HIV protease inhibitors.

Topics & Concepts

Cryptococcus neoformansProteasesProteaseCryptococcosisProtease inhibitor (pharmacology)MicrobiologyCryptococcusAntifungal drugDrugBiologyChemistryVirologyAntifungalBiochemistryEnzymePharmacologyHuman immunodeficiency virus (HIV)Antiretroviral therapyViral loadFungal Infections and StudiesPeptidase Inhibition and AnalysisAntifungal resistance and susceptibility