High-Throughput Chemical Screen Identifies a 2,5-Disubstituted Pyridine as an Inhibitor of Candida albicans Erg11.

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Tytuł:: High-Throughput Chemical Screen Identifies a 2,5-Disubstituted Pyridine as an Inhibitor of Candida albicans Erg11.
Autorzy:: Du Bois AC; Department of Molecular Genetics, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Xue A; Department of Molecular Genetics, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Pham C; Department of Chemical Engineering and Applied Chemistry, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Revie NM; Department of Molecular Genetics, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Meyer KJ; Department of Biochemistry, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Yashiroda Y; RIKENgrid.7597.c Center for Sustainable Resource Science, Wako, Saitama, Japan.
Boone C; Department of Molecular Genetics, University of Torontogrid.17063.33, Toronto, Ontario, Canada.; RIKENgrid.7597.c Center for Sustainable Resource Science, Wako, Saitama, Japan.; Donnelly Centre for Cellular and Biomedical Research, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Nodwell JR; Department of Biochemistry, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Stogios P; Department of Chemical Engineering and Applied Chemistry, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Savchenko A; Department of Chemical Engineering and Applied Chemistry, University of Torontogrid.17063.33, Toronto, Ontario, Canada.; Department of Microbiology, Immunology and Infectious Diseases, Cumming School of Medicine, University of Calgary, Calgary, Alberta, Canada.
Robbins N; Department of Molecular Genetics, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Iyer KR; Department of Molecular Genetics, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Cowen LE; Department of Molecular Genetics, University of Torontogrid.17063.33, Toronto, Ontario, Canada.
Źródło:: MSphere [mSphere] 2022 Jun 29; Vol. 7 (3), pp. e0007522. Date of Electronic Publication: 2022 May 09.
Typ publikacji:: Journal Article; Research Support, Non-U.S. Gov't; Research Support, N.I.H., Extramural
Język:: English
Imprint Name(s):: Original Publication: Washington, DC : American Society for Microbiology, [2015]-
MeSH Terms:: Antifungal Agents*/pharmacology
Antifungal Agents*/therapeutic use
Candida albicans*/genetics
Azoles/pharmacology ; Drug Resistance, Fungal/genetics ; Ergosterol/genetics ; Humans ; Nitrogen ; Pyridines/pharmacology ; Sterols
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Grant Information:: FDN-143264 Canada CIHR; FDN-154288 Canada CIHR; R01 AI120958 United States AI NIAID NIH HHS
Contributed Indexing:: Keywords: 2; 5-disubstituted pyridine; Candida albicans; Erg11; azole; chemogenomics; computational modeling; ergosterol; fungal pathogen
Substance Nomenclature:: 0 (Antifungal Agents)
0 (Azoles)
0 (Pyridines)
0 (Sterols)
N762921K75 (Nitrogen)
Z30RAY509F (Ergosterol)
Entry Date(s):: Date Created: 20220509 Date Completed: 20220701 Latest Revision: 20220722
Update Code:: 20240105
PubMed Central ID:: PMC9241532
DOI:: 10.1128/msphere.00075-22
PMID:: 35531664
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Fungal infections contribute to over 1.5 million deaths annually, with Candida albicans representing one of the most concerning human fungal pathogens. While normally commensal in nature, compromise of host immunity can result in C. albicans disseminating into the human bloodstream, causing infections with mortality rates of up to 40%. A contributing factor to this high mortality rate is the limited arsenal of antifungals approved to treat systemic infections. The most widely used antifungal class, the azoles, inhibits ergosterol biosynthesis by targeting Erg11. The rise of drug resistance among C. albicans clinical isolates, particularly against the azoles, has escalated the need to explore novel antifungal strategies. To address this challenge, we screened a 9,600-compound subset of the University of Tokyo Core Chemical Library to identify molecules with novel antifungal activity against C. albicans. The most potent hit molecule was CpdLC-6888, a 2,5-disubstituted pyridine compound, which inhibited growth of C. albicans and closely-related species. Chemical-genetic, biochemical, and modeling analyses suggest that CpdLC-6888 inhibits Erg11 in a manner similar to the azoles despite lacking the canonical five-membered nitrogen-containing azole ring. This work characterizes the antifungal activity of a 2,5-disubstituted pyridine against C. albicans, supporting the mining of existing chemical collections to identify compounds with novel antifungal activity. IMPORTANCE Pathogenic fungi represent a serious but underacknowledged threat to human health. The treatment and management of these infections relies heavily on the use of azole antifungals, a class of molecules that contain a five-membered nitrogen-containing ring and inhibit the biosynthesis of the key membrane sterol ergosterol. By employing a high-throughput chemical screen, we identified a 2,5-disubstituted pyridine, termed CpdLC-6888, as possessing antifungal activity against the prominent human fungal pathogen Candida albicans. Upon further investigation, we determined this molecule exhibits azole-like activity despite being structurally divergent. Specifically, transcriptional repression of the azole target gene ERG11 resulted in hypersensitivity to CpdLC-6888, and treatment of C. albicans with this molecule blocked the production of the key membrane sterol ergosterol. Therefore, this work describes a chemical scaffold with novel antifungal activity against a prevalent and threatening fungal pathogen affecting human health, expanding the repertoire of compounds that can inhibit this useful antifungal drug target.

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