Immunosuppressive and Nonimmunosuppressive Cyclosporine Analogs Are Toxic to the Opportunistic Fungal Pathogen Cryptococcus neoformans via Cyclophilin-Dependent Inhibition of Calcineurin

Author:

Cruz M. Cristina1,Del Poeta Maurizio23,Wang Ping1,Wenger Roland4,Zenke Gerhard4,Quesniaux Valerie F. J.4,Movva N. Rao4,Perfect John R.52,Cardenas Maria E.1,Heitman Joseph16527

Affiliation:

1. Departments ofGenetics,1

2. Medicine,2 Duke University Medical Center and

3. Institute of Infectious Diseases and Public Health, University of Ancona, Ancona, Italy3; and

4. Novartis, Basel CH-4002, Switzerland4

5. Microbiology,5 and

6. Pharmacology and Cancer Biology,6

7. Howard Hughes Medical Institute,7 Durham, North Carolina 27710;

Abstract

ABSTRACT Cyclosporine (CsA) is an immunosuppressive and antimicrobial drug which, in complex with cyclophilin A, inhibits the protein phosphatase calcineurin. We recently found that Cryptococcus neoformans growth is resistant to CsA at 24°C but sensitive at 37°C and that calcineurin is required for growth at 37°C and pathogenicity. Here CsA analogs were screened for toxicity against C. neoformans in vitro. In most cases, antifungal activity was correlated with cyclophilin A binding in vitro and inhibition of the mixed-lymphocyte reaction and interleukin 2 production in cell culture. Two unusual nonimmunosuppressive CsA derivatives, (γ-OH) MeLeu 4 -Cs (211-810) and D-Sar (α-SMe) 3 Val 2 -DH-Cs (209-825), which are also toxic to C. neoformans were identified. These CsA analogs inhibit C. neoformans via fungal cyclophilin A and calcineurin homologs. Our findings identify calcineurin as a novel antifungal drug target and suggest nonimmunosuppressive CsA analogs warrant investigation as antifungal agents.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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