Abstract
Aspergillus flavus is a pathogenic fungal species that can cause pulmonary aspergillosis, and triazole compounds are used for the treatment of these infections. Prolonged exposure to azoles may select for compensatory mutations in the A. flavus genome, resulting in azole resistance. Here, we characterize a series of 11 isogenic A. flavus strains isolated from a patient with pulmonary as-pergillosis. Over a period of three months, the initially azole-susceptible strain developed itracona-zole and voriconazole resistance. Short tandem repeat analysis and whole-genome sequencing revealed the high genetic relatedness of all isolates, indicating an infection with one single isolate. In contrast, the isolates were macroscopically highly diverse, suggesting an adaptation to the environment due to (epi)genetic changes. The whole-genome sequencing of susceptible and azole-resistant strains showed a number of mutations that might be associated with azole resistance. The majority of resistant strains contain a Y119F mutation in the Cyp51A gene, which corresponds to the Y121F mutation found in A. fumigatus. One azole-resistant strain demonstrated a divergent set of muta-tions, including a V99A mutation in a major facilitator superfamily (MSF) multidrug transporter (AFLA 083950).
Original language | English |
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Pages (from-to) | 1-17 |
Number of pages | 17 |
Journal | Journal of Fungi |
Volume | 7 |
DOIs | |
Publication status | Published - 2021 |
Keywords
- Acquired resistance
- Aspergillosis
- Azole resistance
- Chronic pulmonary aspergillosis
- Cyp51A
- Y119F