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A Tetraploid Intermediate Precedes Aneuploid Formation in Yeasts Exposed to Fluconazole

Candida albicans, the most prevalent human fungal pathogen, is generally diploid. However, 50% of isolates that are resistant to fluconazole (FLC), the most widely used antifungal, are aneuploid and some aneuploidies can confer FLC resistance. To ask if FLC exposure causes or only selects for aneupl...

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Autores principales: Harrison, Benjamin D., Hashemi, Jordan, Bibi, Maayan, Pulver, Rebecca, Bavli, Danny, Nahmias, Yaakov, Wellington, Melanie, Sapiro, Guillermo, Berman, Judith
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3958355/
https://www.ncbi.nlm.nih.gov/pubmed/24642609
http://dx.doi.org/10.1371/journal.pbio.1001815
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author Harrison, Benjamin D.
Hashemi, Jordan
Bibi, Maayan
Pulver, Rebecca
Bavli, Danny
Nahmias, Yaakov
Wellington, Melanie
Sapiro, Guillermo
Berman, Judith
author_facet Harrison, Benjamin D.
Hashemi, Jordan
Bibi, Maayan
Pulver, Rebecca
Bavli, Danny
Nahmias, Yaakov
Wellington, Melanie
Sapiro, Guillermo
Berman, Judith
author_sort Harrison, Benjamin D.
collection PubMed
description Candida albicans, the most prevalent human fungal pathogen, is generally diploid. However, 50% of isolates that are resistant to fluconazole (FLC), the most widely used antifungal, are aneuploid and some aneuploidies can confer FLC resistance. To ask if FLC exposure causes or only selects for aneuploidy, we analyzed diploid strains during exposure to FLC using flow cytometry and epifluorescence microscopy. FLC exposure caused a consistent deviation from normal cell cycle regulation: nuclear and spindle cycles initiated prior to bud emergence, leading to “trimeras,” three connected cells composed of a mother, daughter, and granddaughter bud. Initially binucleate, trimeras underwent coordinated nuclear division yielding four daughter nuclei, two of which underwent mitotic collapse to form a tetraploid cell with extra spindle components. In subsequent cell cycles, the abnormal number of spindles resulted in unequal DNA segregation and viable aneuploid progeny. The process of aneuploid formation in C. albicans is highly reminiscent of early stages in human tumorigenesis in that aneuploidy arises through a tetraploid intermediate and subsequent unequal DNA segregation driven by multiple spindles coupled with a subsequent selective advantage conferred by at least some aneuploidies during growth under stress. Finally, trimera formation was detected in response to other azole antifungals, in related Candida species, and in an in vivo model for Candida infection, suggesting that aneuploids arise due to azole treatment of several pathogenic yeasts and that this can occur during the infection process.
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spelling pubmed-39583552014-03-27 A Tetraploid Intermediate Precedes Aneuploid Formation in Yeasts Exposed to Fluconazole Harrison, Benjamin D. Hashemi, Jordan Bibi, Maayan Pulver, Rebecca Bavli, Danny Nahmias, Yaakov Wellington, Melanie Sapiro, Guillermo Berman, Judith PLoS Biol Research Article Candida albicans, the most prevalent human fungal pathogen, is generally diploid. However, 50% of isolates that are resistant to fluconazole (FLC), the most widely used antifungal, are aneuploid and some aneuploidies can confer FLC resistance. To ask if FLC exposure causes or only selects for aneuploidy, we analyzed diploid strains during exposure to FLC using flow cytometry and epifluorescence microscopy. FLC exposure caused a consistent deviation from normal cell cycle regulation: nuclear and spindle cycles initiated prior to bud emergence, leading to “trimeras,” three connected cells composed of a mother, daughter, and granddaughter bud. Initially binucleate, trimeras underwent coordinated nuclear division yielding four daughter nuclei, two of which underwent mitotic collapse to form a tetraploid cell with extra spindle components. In subsequent cell cycles, the abnormal number of spindles resulted in unequal DNA segregation and viable aneuploid progeny. The process of aneuploid formation in C. albicans is highly reminiscent of early stages in human tumorigenesis in that aneuploidy arises through a tetraploid intermediate and subsequent unequal DNA segregation driven by multiple spindles coupled with a subsequent selective advantage conferred by at least some aneuploidies during growth under stress. Finally, trimera formation was detected in response to other azole antifungals, in related Candida species, and in an in vivo model for Candida infection, suggesting that aneuploids arise due to azole treatment of several pathogenic yeasts and that this can occur during the infection process. Public Library of Science 2014-03-18 /pmc/articles/PMC3958355/ /pubmed/24642609 http://dx.doi.org/10.1371/journal.pbio.1001815 Text en © 2014 Harrison et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Harrison, Benjamin D.
Hashemi, Jordan
Bibi, Maayan
Pulver, Rebecca
Bavli, Danny
Nahmias, Yaakov
Wellington, Melanie
Sapiro, Guillermo
Berman, Judith
A Tetraploid Intermediate Precedes Aneuploid Formation in Yeasts Exposed to Fluconazole
title A Tetraploid Intermediate Precedes Aneuploid Formation in Yeasts Exposed to Fluconazole
title_full A Tetraploid Intermediate Precedes Aneuploid Formation in Yeasts Exposed to Fluconazole
title_fullStr A Tetraploid Intermediate Precedes Aneuploid Formation in Yeasts Exposed to Fluconazole
title_full_unstemmed A Tetraploid Intermediate Precedes Aneuploid Formation in Yeasts Exposed to Fluconazole
title_short A Tetraploid Intermediate Precedes Aneuploid Formation in Yeasts Exposed to Fluconazole
title_sort tetraploid intermediate precedes aneuploid formation in yeasts exposed to fluconazole
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3958355/
https://www.ncbi.nlm.nih.gov/pubmed/24642609
http://dx.doi.org/10.1371/journal.pbio.1001815
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