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Centromere deletion in Cryptococcus deuterogattii leads to neocentromere formation and chromosome fusions.


ABSTRACT: The human fungal pathogen Cryptococcus deuterogattii is RNAi-deficient and lacks active transposons in its genome. C. deuterogattii has regional centromeres that contain only transposon relics. To investigate the impact of centromere loss on the C. deuterogattii genome, either centromere 9 or 10 was deleted. Deletion of either centromere resulted in neocentromere formation and interestingly, the genes covered by these neocentromeres maintained wild-type expression levels. In contrast to cen9? mutants, cen10? mutant strains exhibited growth defects and were aneuploid for chromosome 10. At an elevated growth temperature (37°C), the cen10? chromosome was found to have undergone fusion with another native chromosome in some isolates and this fusion restored wild-type growth. Following chromosomal fusion, the neocentromere was inactivated, and the native centromere of the fused chromosome served as the active centromere. The neocentromere formation and chromosomal fusion events observed in this study in C. deuterogattii may be similar to events that triggered genomic changes within the Cryptococcus/Kwoniella species complex and may contribute to speciation throughout the eukaryotic domain.

SUBMITTER: Schotanus K 

PROVIDER: S-EPMC7188483 | biostudies-literature | 2020 Apr

REPOSITORIES: biostudies-literature

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Centromere deletion in <i>Cryptococcus deuterogattii</i> leads to neocentromere formation and chromosome fusions.

Schotanus Klaas K   Heitman Joseph J  

eLife 20200420


The human fungal pathogen <i>Cryptococcus deuterogattii</i> is RNAi-deficient and lacks active transposons in its genome. <i>C. deuterogattii</i> has regional centromeres that contain only transposon relics. To investigate the impact of centromere loss on the <i>C. deuterogattii</i> genome, either centromere 9 or 10 was deleted. Deletion of either centromere resulted in neocentromere formation and interestingly, the genes covered by these neocentromeres maintained wild-type expression levels. In  ...[more]

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