Journal of Fungi (Jan 2024)

Role of the <i>osaA</i> Gene in <i>Aspergillus fumigatus</i> Development, Secondary Metabolism and Virulence

  • Apoorva Dabholkar,
  • Sandesh Pandit,
  • Ritu Devkota,
  • Sourabh Dhingra,
  • Sophie Lorber,
  • Olivier Puel,
  • Ana M. Calvo

DOI
https://doi.org/10.3390/jof10020103
Journal volume & issue
Vol. 10, no. 2
p. 103

Abstract

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Aspergillus fumigatus is the leading cause of aspergillosis, associated with high mortality rates, particularly in immunocompromised individuals. In search of novel genetic targets against aspergillosis, we studied the WOPR transcription factor OsaA. The deletion of the osaA gene resulted in colony growth reduction. Conidiation is also influenced by osaA; both osaA deletion and overexpression resulted in a decrease in spore production. Wild-type expression levels of osaA are necessary for the expression of the conidiation regulatory genes brlA, abaA, and wetA. In addition, osaA is necessary for normal cell wall integrity. Furthermore, the deletion of osaA resulted in a reduction in the ability of A. fumigatus to adhere to surfaces, decreased thermotolerance, as well as increased sensitivity to oxidative stress. Metabolomics analysis indicated that osaA deletion or overexpression led to alterations in the production of multiple secondary metabolites, including gliotoxin. This was accompanied by changes in the expression of genes in the corresponding secondary metabolite gene clusters. These effects could be, at least in part, due to the observed reduction in the expression levels of the veA and laeA global regulators when the osaA locus was altered. Importantly, our study shows that osaA is indispensable for virulence in both neutropenic and corticosteroid-immunosuppressed mouse models.

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