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In Vitro Resistance Selections for Plasmodium falciparum Dihydroorotate Dehydrogenase Inhibitors Give Mutants with Multiple Point Mutations in the Drug-binding Site and Altered Growth
Authors:Leila S. Ross  Francisco Javier Gamo  Maria José Lafuente-Monasterio  Onkar M. P. Singh  Paul Rowland  Roger C. Wiegand  Dyann F. Wirth
Affiliation:From the Department of Immunology and Infectious Diseases, Harvard School of Public Health, Boston, Massachusetts 02115.;the §Tres Cantos Medicines Development Campus, GlaxoSmithKline, 28760 Tres Cantos, Madrid, Spain.;the Computational and Structural Chemistry, GlaxoSmithKline, Stevenage, Hertfordshire SG1 2NY, United Kingdom, and ;the Infectious Disease Initiative, Broad Institute, Cambridge, Massachusetts 02142
Abstract:Malaria is a preventable and treatable disease; yet half of the world''s population lives at risk of infection, and an estimated 660,000 people die of malaria-related causes every year. Rising drug resistance threatens to make malaria untreatable, necessitating both the discovery of new antimalarial agents and the development of strategies to identify and suppress the emergence and spread of drug resistance. We focused on in-development dihydroorotate dehydrogenase (DHODH) inhibitors. Characterizing resistance pathways for antimalarial agents not yet in clinical use will increase our understanding of the potential for resistance. We identified resistance mechanisms of Plasmodium falciparum (Pf) DHODH inhibitors via in vitro resistance selections. We found 11 point mutations in the PfDHODH target. Target gene amplification and unknown mechanisms also contributed to resistance, albeit to a lesser extent. These mutant parasites were often hypersensitive to other PfDHODH inhibitors, which immediately suggested a novel combination therapy approach to preventing resistance. Indeed, a combination of wild-type and mutant-type selective inhibitors led to resistance far less often than either drug alone. The effects of point mutations in PfDHODH were corroborated with purified recombinant wild-type and mutant-type PfDHODH proteins, which showed the same trends in drug response as the cognate cell lines. Comparative growth assays demonstrated that two mutant parasites grew less robustly than their wild-type parent, and the purified protein of those mutants showed a decrease in catalytic efficiency, thereby suggesting a reason for the diminished growth rate. Co-crystallography of PfDHODH with three inhibitors suggested that hydrophobic interactions are important for drug binding and selectivity.
Keywords:Drug Resistance   Evolution   Infectious Disease   Malaria   Nucleotide   Pyrimidine
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