4.4 Article

Population genetics and microevolution of clinical Candida glabrata reveals recombinant sequence types and hyper-variation within mitochondrial genomes, virulence genes, and drug targets

Journal

GENETICS
Volume 221, Issue 1, Pages -

Publisher

GENETICS SOCIETY AMERICA
DOI: 10.1093/genetics/iyac031

Keywords

Candida glabrata; genome sequencing; epidemiology; candidiasis; microevolution; mitochondria; drug-resistance; evolution

Funding

  1. Medical Research Council Centre for Medical Mycology [MR/N006364/2]
  2. Wellcome Trust Seed Award [215239/Z/19/Z]
  3. Wellcome Trust Senior Research Fellowship [214317/Z/18/Z]
  4. European Union [812969]
  5. consortium 'Host-Directed Medicine in invasive FUNgal infections'-HDM-FUN [847507]
  6. Wellcome Trust [215239/Z/19/Z, 214317/Z/18/Z] Funding Source: Wellcome Trust

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This study reveals the high genetic diversity of C. glabrata clinical isolates in Scotland, including multiple previously identified sequence types from around the world and a newly discovered sequence type. Ancient recombination events were found between different geographical regions, suggesting transmission and genetic exchange. The study also identifies genetic variations and microevolution related to drug resistance and virulence.
Candida glabrata is the second most common etiological cause of worldwide systemic candidiasis in adult patients. Genome analysis of 68 isolates from 8 hospitals across Scotland, together with 83 global isolates, revealed insights into the population genetics and evolution of C. glabrata. Clinical isolates of C. glabrata from across Scotland are highly genetically diverse, including at least 19 separate sequence types that have been recovered previously in globally diverse locations, and 1 newly discovered sequence type. Several sequence types had evidence for ancestral recombination, suggesting transmission between distinct geographical regions has coincided with genetic exchange arising in new clades. Three isolates were missing MAT alpha 1, potentially representing a second mating type. Signatures of positive selection were identified in every sequence type including enrichment for epithelial adhesins thought to facilitate fungal adhesin to human epithelial cells. In patent microevolution was identified from 7 sets of recurrent cases of candidiasis, revealing an enrichment for nonsynonymous and frameshift indels in cell surface proteins. Microevolution within patients also affected epithelial adhesins genes, and several genes involved in drug resistance including the ergosterol synthesis gene ERG4 and the echinocandin target FKS1/2, the latter coinciding with a marked drop in fluconazole minimum inhibitory concentration. In addition to nuclear genome diversity, the C. glabrata mitochondrial genome was particularly diverse, with reduced conserved sequence and conserved protein-encoding genes in all nonreference ST15 isolates. Together, this study highlights the genetic diversity within the C. glabrata population that may impact virulence and drug resistance, and 2 major mechanisms generating this diversity: microevolution and genetic exchange/recombination.

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