Enhanced fungal specificity and in vivo therapeutic efficacy of a C-22-modified FK520 analog against C. neoformans

Fungal infections are of mounting global concern, and the current limited treatment arsenal poses challenges when treating such infections. In particular, infections by Cryptococcus neoformans are associated with high mortality, emphasizing the need for novel therapeutic options. Calcineurin is a pr...

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Autores principales: Rivera, Angela, Young Lim, Won, Park, Eunchong, Dome, Patrick A., Hoy, Michael J., Spasojevic, Ivan, Sun, Sheng, Averette, Anna Floyd, Pina-Oviedo, Sergio, Juvvadi, Praveen R., Steinbach, William J., Ciofani, Maria, Hong, Jiyong, Heitman, Joseph
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10653846/
https://www.ncbi.nlm.nih.gov/pubmed/37737622
http://dx.doi.org/10.1128/mbio.01810-23
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author Rivera, Angela
Young Lim, Won
Park, Eunchong
Dome, Patrick A.
Hoy, Michael J.
Spasojevic, Ivan
Sun, Sheng
Averette, Anna Floyd
Pina-Oviedo, Sergio
Juvvadi, Praveen R.
Steinbach, William J.
Ciofani, Maria
Hong, Jiyong
Heitman, Joseph
author_facet Rivera, Angela
Young Lim, Won
Park, Eunchong
Dome, Patrick A.
Hoy, Michael J.
Spasojevic, Ivan
Sun, Sheng
Averette, Anna Floyd
Pina-Oviedo, Sergio
Juvvadi, Praveen R.
Steinbach, William J.
Ciofani, Maria
Hong, Jiyong
Heitman, Joseph
author_sort Rivera, Angela
collection PubMed
description Fungal infections are of mounting global concern, and the current limited treatment arsenal poses challenges when treating such infections. In particular, infections by Cryptococcus neoformans are associated with high mortality, emphasizing the need for novel therapeutic options. Calcineurin is a protein phosphatase that mediates fungal stress responses, and calcineurin inhibition by the natural product FK506 blocks C. neoformans growth at 37°C. Calcineurin is also required for pathogenesis. However, because calcineurin is conserved in humans and inhibition with FK506 results in immunosuppression, the use of FK506 as an anti-infective agent is precluded. We previously elucidated the structures of multiple fungal calcineurin-FK506-FKBP12 complexes and implicated the C-22 position on FK506 as a key point for differential modification of ligand inhibition of mammalian versus fungal target proteins. Through in vitro antifungal and immunosuppressive testing of FK520 (a natural analog of FK506) derivatives, we identified JH-FK-08 as a lead candidate for further antifungal development. JH-FK-08 exhibited significantly reduced immunosuppressive activity and both reduced fungal burden and prolonged survival of infected animals. JH-FK-08 exhibited additive activity in combination with fluconazole in vivo. These findings further advance calcineurin inhibition as an antifungal therapeutic approach. IMPORTANCE: Fungal infections cause significant morbidity and mortality globally. The therapeutic armamentarium against these infections is limited, and the development of antifungal drugs has been hindered by the evolutionary conservation between fungi and the human host. With rising resistance to the current antifungal arsenal and an increasing at-risk population, there is an urgent need for the development of new antifungal compounds. The FK520 analogs described in this study display potent antifungal activity as a novel class of antifungals centered on modifying an existing orally active FDA-approved therapy. This research advances the development of much-needed newer antifungal treatment options with novel mechanisms of action.
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spelling pubmed-106538462023-09-22 Enhanced fungal specificity and in vivo therapeutic efficacy of a C-22-modified FK520 analog against C. neoformans Rivera, Angela Young Lim, Won Park, Eunchong Dome, Patrick A. Hoy, Michael J. Spasojevic, Ivan Sun, Sheng Averette, Anna Floyd Pina-Oviedo, Sergio Juvvadi, Praveen R. Steinbach, William J. Ciofani, Maria Hong, Jiyong Heitman, Joseph mBio Research Article Fungal infections are of mounting global concern, and the current limited treatment arsenal poses challenges when treating such infections. In particular, infections by Cryptococcus neoformans are associated with high mortality, emphasizing the need for novel therapeutic options. Calcineurin is a protein phosphatase that mediates fungal stress responses, and calcineurin inhibition by the natural product FK506 blocks C. neoformans growth at 37°C. Calcineurin is also required for pathogenesis. However, because calcineurin is conserved in humans and inhibition with FK506 results in immunosuppression, the use of FK506 as an anti-infective agent is precluded. We previously elucidated the structures of multiple fungal calcineurin-FK506-FKBP12 complexes and implicated the C-22 position on FK506 as a key point for differential modification of ligand inhibition of mammalian versus fungal target proteins. Through in vitro antifungal and immunosuppressive testing of FK520 (a natural analog of FK506) derivatives, we identified JH-FK-08 as a lead candidate for further antifungal development. JH-FK-08 exhibited significantly reduced immunosuppressive activity and both reduced fungal burden and prolonged survival of infected animals. JH-FK-08 exhibited additive activity in combination with fluconazole in vivo. These findings further advance calcineurin inhibition as an antifungal therapeutic approach. IMPORTANCE: Fungal infections cause significant morbidity and mortality globally. The therapeutic armamentarium against these infections is limited, and the development of antifungal drugs has been hindered by the evolutionary conservation between fungi and the human host. With rising resistance to the current antifungal arsenal and an increasing at-risk population, there is an urgent need for the development of new antifungal compounds. The FK520 analogs described in this study display potent antifungal activity as a novel class of antifungals centered on modifying an existing orally active FDA-approved therapy. This research advances the development of much-needed newer antifungal treatment options with novel mechanisms of action. American Society for Microbiology 2023-09-22 /pmc/articles/PMC10653846/ /pubmed/37737622 http://dx.doi.org/10.1128/mbio.01810-23 Text en Copyright © 2023 Rivera et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Rivera, Angela
Young Lim, Won
Park, Eunchong
Dome, Patrick A.
Hoy, Michael J.
Spasojevic, Ivan
Sun, Sheng
Averette, Anna Floyd
Pina-Oviedo, Sergio
Juvvadi, Praveen R.
Steinbach, William J.
Ciofani, Maria
Hong, Jiyong
Heitman, Joseph
Enhanced fungal specificity and in vivo therapeutic efficacy of a C-22-modified FK520 analog against C. neoformans
title Enhanced fungal specificity and in vivo therapeutic efficacy of a C-22-modified FK520 analog against C. neoformans
title_full Enhanced fungal specificity and in vivo therapeutic efficacy of a C-22-modified FK520 analog against C. neoformans
title_fullStr Enhanced fungal specificity and in vivo therapeutic efficacy of a C-22-modified FK520 analog against C. neoformans
title_full_unstemmed Enhanced fungal specificity and in vivo therapeutic efficacy of a C-22-modified FK520 analog against C. neoformans
title_short Enhanced fungal specificity and in vivo therapeutic efficacy of a C-22-modified FK520 analog against C. neoformans
title_sort enhanced fungal specificity and in vivo therapeutic efficacy of a c-22-modified fk520 analog against c. neoformans
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10653846/
https://www.ncbi.nlm.nih.gov/pubmed/37737622
http://dx.doi.org/10.1128/mbio.01810-23
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