Azole resistance in Aspergillus flavus and associated fitness cost

Author:

Djenontin Elie12,Debourgogne Anne3,Mousavi Bita2,Delhaes Laurence4,Cornet Muriel5,Valsecchi Isabel1,Adebo Makiath2,Guillot Jacques6ORCID,Botterel Françoise12,Dannaoui Eric178

Affiliation:

1. Unité de Parasitologie‐Mycologie, Département de Virologie, Bactériologie‐Hygiène, Parasitologie‐Mycologie CHU Henri Mondor, AP‐HP Créteil France

2. UR Dynamyc UPEC, EnvA, ANSES. Faculté de Santé de Créteil Créteil France

3. UR7300 Stress Immunité Pathogène, Université de Lorraine Vandoeuvre les Nancy France

4. CHU de Bordeaux: Laboratoire de Parasitologie‐Mycologie, CNR des Aspergilloses Chroniques, INSERM U1045: Univ. Bordeaux Bordeaux France

5. Université Grenoble Alpes, CNRS, Grenoble INP, CHU Grenoble Alpes, TIMC Grenoble France

6. Oniris, VetAgroBio Nantes Nantes France

7. Unité de Parasitologie‐Mycologie, Service de Microbiologie, Hôpital Necker, AP‐HP Paris France

8. Université Paris Cité Faculté de Médecine Paris France

Abstract

AbstractBackgroundThe resistance of Aspergillus flavus to the azole antifungal drugs is an emerging problem. Mutations in the molecular targets of the azole antifungals ‐ CYP 51 A, B and C ‐ are possible mechanisms of resistance, but data to confirm this hypothesis are scarce. In addition, the behaviour of resistant strains in vitro and in vivo is not yet understood.ObjectivesThis study had 3 objectives. The first was to compare the sequences of CYP51 A, B and C in resistant and susceptible strains of A. flavus. The second was to look for the existence of a fitness cost associated with resistance. The third was to evaluate the activity of voriconazole and posaconazole on resistant strains in the Galleria mellonella model.MethodsThe CYP51 A, B and C sequences of seven resistant strains with those of four susceptible strains are compared. Fitness costs were assessed by growing the strains in RPMI medium and testing their virulence in G. mellonella larvae. In addition, G. mellonella larvae infected with strains of A. flavus were treated with voriconazole and posaconazole.ResultsIn the CYP51A sequences, we found the A91T, C708T and A1296T nucleotide substitutions only in the resistant strains. The resistant strains showed a fitness cost with reduced in vitro growth and reduced virulence in G. mellonella. In vivo resistance to posaconazole is confirmed in a strain with the highest MIC for this antifungal agent.ConclusionsThese results allow to conclude that some substitutions in CYP51 genes, in particular CYP51A, contribute to resistance to azole drugs in A. flavus. The study of the relationship between drug dosage and treatment duration with resistance and the reduction of fitness costs in resistant strains is a major perspective of this study. This work could help to establish recommendations for the treatment of infections with resistant strains of A. flavus.

Publisher

Wiley

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