In vitro small molecule screening to inform novel candidates for use in fluconazole combination therapy in vivo against Coccidioides

Heather L. Mead; Michael Valentine; Holly Yin; George R. Thompson III; Paul Keim; David M. Engelthaler; Bridget M. Barker

doi:10.1128/spectrum.01008-24

Microbiology Spectrum (Oct 2024)

In vitro small molecule screening to inform novel candidates for use in fluconazole combination therapy in vivo against Coccidioides

Heather L. Mead,
Michael Valentine,
Holly Yin,
George R. Thompson III,
Paul Keim,
David M. Engelthaler,
Bridget M. Barker

Affiliations

Heather L. Mead: The Translational Genomics Research Institute North, Flagstaff, Arizona, USA
Michael Valentine: The Translational Genomics Research Institute North, Flagstaff, Arizona, USA
Holly Yin: Beckman Research Institute of the City of Hope, Duarte, California, USA
George R. Thompson III: Department of Internal Medicine, Division of Infectious Diseases, University of California-Davis, Sacramento, California, USA
Paul Keim: Department of Biological Sciences, The Pathogen and Microbiome Institute, Northern Arizona University, Flagstaff, Arizona, USA
David M. Engelthaler: The Translational Genomics Research Institute North, Flagstaff, Arizona, USA
Bridget M. Barker: Department of Biological Sciences, The Pathogen and Microbiome Institute, Northern Arizona University, Flagstaff, Arizona, USA

DOI: https://doi.org/10.1128/spectrum.01008-24
Journal volume & issue: Vol. 12, no. 10

Abstract

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ABSTRACT Identifying improved treatments for severe and refractory coccidioidomycosis (Valley fever) is needed. This endemic fungal disease is common in North and South America, and cases have increased substantially over the last 30 years. The current standard of care, oral daily fluconazole, often fails to completely eradicate Coccidioides infection; however, the high cost of identifying new compounds effective in treating Valley fever is a barrier to improving treatment. Therefore, repurposing existing pharmaceutical agents in combination with fluconazole therapy is an attractive option. We screened the Library of Pharmacologically Active Compounds (LOPAC) small molecule library for compounds that inhibited fungal growth in vitro and determined IC50 values for a subset of compounds. Based on these findings, we tested a small subset of these agents to validate the screen, as well as to test the performance of fluconazole in a combination therapy approach, as compared with fluconazole alone, in a murine model. We observed that combination therapy of tamoxifen:fluconazole and sertraline:fluconazole significantly reduced the burden of live fungus in the lung compared with fluconazole alone, and we observed reduced or nonexistent dissemination. These results suggest that tamoxifen and sertraline may be repurposed as adjunctive agents in the treatment of this important fungal disease.IMPORTANCEDeveloping new drugs, especially for regional orphan diseases, such as Valley Fever, is a slow and costly endeavor. However, there is a wealth of FDA-approved drugs available for repurposing, offering a more economical and expedited approach to improve treatment. Those existing compounds with antifungal properties can become novel therapies with relative ease: a considerable advantage for patients in need of alternative treatment. Despite the scope of remaining tasks, our comprehensive screening of potential candidates has revealed promising combinations for further exploration. This effort outlines a practical pipeline for Valley fever drug screening and identifies viable drug combinations that could impact patients more rapidly than single drug development pathways.

Published in Microbiology Spectrum

ISSN: 2165-0497 (Online)
Publisher: American Society for Microbiology
Country of publisher: United States
LCC subjects: Science: Microbiology
Website: https://journals.asm.org/journal/spectrum

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