Abstract

Transdisciplinary Program to Identify Novel Antifungal Targets This Program Project represents a unique, coordinated and synergistic strategy to discover novel antifungal drugs to effectively treat life-threatening invasive fungal infections. Invasive fungal infections remain a leading cause of death in the growing population of immunosuppressed patients. Presently, there are several classes of approved antifungal agents, but they suffer from limited clinical efficacy, reduced fungicidal activity in the host, debilitating toxicity profiles, and/or emergence of resistance. To identify innovative antifungal targets and agents, we have merged the disciplines of structural biology, molecular mycology, and vertebrate pathology with our clinical insights and experience to produce a novel direction for antifungal development. This focus targets three cell signaling pathways critical to the capability of pathogenic fungi to survive and grow at human body temperature (37C). Our previous studies have identified and carefully validated these signal transduction circuits that enable high temperature growth at 37C and virulence for the three major fungal pathogens (Candida, Aspergillus, Cryptococcus). These three pathways are: (1) the calcineurin pathway, a conserved pathway for fungal virulence; (2) the Ras pathway, which governs fungal morphogenesis and stress responses; and (3) the trehalose pathway, which synthesizes a fungal specific thermoprotective carbohydrate and other stress protectants. Our work to date has also identified key interconnections among these pathways, which we will further investigate for synergistic therapeutic potential. Our overall hypothesis is that by applying structural biologc approaches to rigorous investigations in mycology, we will define critical, targetable differences between key fungal proteins required for thermotolerance and the proteins' mammalian counterparts, creating a therapeutic platform on which to develop novel fungal-specific inhibitors that lack mammalian cross-reactivity. Our overall aims are to: (1) define fungal-specific structural differences in the three signaling pathways, (2) generate novel inhibitors against these signaling pathways and optimize their entry into fungal cells, and (3) test inhibitors for in vitro and in vivo biological activity. To accomplish these Aims, we propose three linked Projects and three supporting Cores. The impact of this novel approach will be to identify and validate potent fungal-specific inhibitors of these critical signaling pathways that can be further translated for clinical application by our industry collaborators to drugs to improve patient outcome.

Public Health Relevance

Transdisciplinary Program to Identify Novel Antifungal Targets Fungal infections are deadly for thousands of people each year, resulting in significant personal and health care burden. In addition, these infections are increasing in prevalence and becoming resistant to existing treatments. The purpose of this Program Project is to understand fungal biology, in particular, three signaling pathways that fungi require to grow within the human body. This information will be used to develop new drugs that specifically block these pathways and lead to fungal death. The Program's ultimate goal is to develop drugs that can be used alone or with existing antifungal treatments to improve patient outcomes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI104533-05
Application #
9709214
Study Section
Special Emphasis Panel (ZAI1)
Program Officer
Love, Dona
Project Start
2015-06-25
Project End
2020-05-31
Budget Start
2019-06-01
Budget End
2020-05-31
Support Year
5
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Duke University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
044387793
City
Durham
State
NC
Country
United States
Zip Code
27705

  Publications

Pianalto, Kaila M; Ost, Kyla S; Brown, Hannah E et al. (2018) Characterization of additional components of the environmental pH-sensing complex in the pathogenic fungus Cryptococcus neoformans. J Biol Chem 293:9995-10008
Brandão, Fabiana; Esher, Shannon K; Ost, Kyla S et al. (2018) HDAC genes play distinct and redundant roles in Cryptococcus neoformans virulence. Sci Rep 8:5209
Lee, Yeonseon; Lee, Kyung-Tae; Lee, Soo Jung et al. (2018) In Vitro and In Vivo Assessment of FK506 Analogs as Novel Antifungal Drug Candidates. Antimicrob Agents Chemother 62:
Esher, Shannon K; Zaragoza, Oscar; Alspaugh, James Andrew (2018) Cryptococcal pathogenic mechanisms: a dangerous trip from the environment to the brain. Mem Inst Oswaldo Cruz 113:e180057
Brown, Hannah E; Ost, Kyla S; Esher, Shannon K et al. (2018) Identifying a novel connection between the fungal plasma membrane and pH-sensing. Mol Microbiol 109:474-493
Perfect, John R; Tenor, Jennifer L; Miao, Yi et al. (2017) Trehalose pathway as an antifungal target. Virulence 8:143-149
Kwon-Chung, Kyung J; Bennett, John E; Wickes, Brian L et al. (2017) The Case for Adopting the ""Species Complex"" Nomenclature for the Etiologic Agents of Cryptococcosis. mSphere 2:
Billmyre, R Blake; Heitman, Joseph (2017) Genetic and epigenetic engines of diversity in pathogenic microbes. PLoS Pathog 13:e1006468
Juvvadi, Praveen R; Lee, Soo Chan; Heitman, Joseph et al. (2017) Calcineurin in fungal virulence and drug resistance: Prospects for harnessing targeted inhibition of calcineurin for an antifungal therapeutic approach. Virulence 8:186-197
Alspaugh, J Andrew (2017) Targeting protein localization for anti-infective therapy. Virulence 8:1105-1107

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