In Vitro Killing Activities of Anidulafungin and Micafungin with and without Nikkomycin Z against Four Candida auris Clades

Awid Adnan; Andrew M Borman; Zoltán Tóth; Lajos Forgács; Renátó Kovács; Dávid Balázsi; Bence Balázs; Gergely Udvarhelyi; Gábor Kardos; László Majoros

doi:10.3390/pharmaceutics15051365

In Vitro Killing Activities of Anidulafungin and Micafungin with and without Nikkomycin Z against Four Candida auris Clades

Pharmaceutics. 2023 Apr 29;15(5):1365. doi: 10.3390/pharmaceutics15051365.

Authors

Awid Adnan^{1

2}, Andrew M Borman^{3

4}, Zoltán Tóth¹, Lajos Forgács^{1

2}, Renátó Kovács¹, Dávid Balázsi^{1

2}, Bence Balázs¹, Gergely Udvarhelyi^{1

2}, Gábor Kardos⁵, László Majoros¹

Affiliations

¹ Department of Medical Microbiology, Faculty of Medicine, University of Debrecen, 4032 Debrecen, Hungary.
² Doctoral School of Pharmaceutical Sciences, University of Debrecen, 4032 Debrecen, Hungary.
³ UK National Mycology Reference Laboratory, UK Health Security Agency, Science Quarter, Southmead Hospital, Bristol BS10 5NB, UK.
⁴ Medical Research Council Centre for Medical Mycology (MRC CMM), University of Exeter, Exeter EX4 4QD, UK.
⁵ Department of Metagenomics, University of Debrecen, 4032 Debrecen, Hungary.

Abstract

Candida auris is a multidrug-resistant pathogen against which echinocandins are the drug of choice. However, information on how the chitin synthase inhibitor nikkomycin Z influences the killing activities of echinocandins against C. auris is currently lacking. We determined the killing activities of anidulafungin and micafungin (0.25, 1, 8, 16 and 32 mg/L each) with and without nikkomycin Z (8 mg/L) against 15 isolates representing four C. auris clades (South Asian n = 5; East Asian n = 3; South African n = 3; South American n = 4, two of which were of environmental origin). Two and one isolates from the South Asian clade harbored mutations in the hot-spot 1 (S639Y and S639P) and 2 (R1354H) regions of the FKS1 gene, respectively. The anidulafungin, micafungin and nikkomycin Z MIC ranges were 0.015-4, 0.03-4 and 2->16 mg/L, respectively. Anidulafungin and micafungin alone exerted weak fungistatic activity against wild-type isolates and the isolate with a mutation in the hot-spot 2 region of FKS1 but was ineffective against the isolates with a mutation in the hot-spot 1 region. The nikkomycin Z killing curves were always similar to their respective controls. Twenty-two of sixty (36.7%) anidulafungin plus nikkomycin Z and twenty-four of sixty (40%) micafungin plus nikkomycin Z combinations produced at least 100-fold decreases in the CFUs (synergy), with a 41.7% and 20% fungicidal effect, respectively, against wild-type isolates. Antagonism was never observed. Similar results were found with the isolate with a mutation in hot-spot 2 of FKS1, but the combinations were ineffective against the two isolates with prominent mutations in hot-spot 1 of FKS1. The simultaneous inhibition of β-1,3 glucan and chitin synthases in wild-type C. auris isolates produced significantly greater killing rates than either drug alone. Further studies are warranted to verify the clinical efficacy of echinocandin plus nikkomycin Z combinations against echinocandin susceptible C. auris isolates.

Keywords: chitin synthase inhibitor; echinocandins; synergism; time–kill methodology.

Grants and funding

NKFIH FK138462/Hungarian National Research, Development and Innovation Office