The influence of a copper efflux pump in Histoplasma capsulatum virulence

Author:

Moraes Dayane1,Tristão Gabriel Brum1,Rappleye Chad A.2,Ray Stephanie C.2,Ribeiro‐Dias Fátima3,Gomes Rodrigo Saar3,Assunção Leandro do Prado1,Paccez Juliano Domiraci1,Zancopé‐Oliveira Rosely Maria4,Silva‐Bailão Mirelle Garcia1,Soares Célia Maria de Almeida1,Bailão Alexandre Melo1ORCID

Affiliation:

1. Laboratório de Biologia Molecular (LBM), Instituto de Ciências Biológicas Universidade Federal de Goiás Goiânia Brazil

2. Department of Microbiology Ohio State University Columbus OH USA

3. Laboratório de Imunidade Natural (LIN), Instituto de Patologia Tropical e Saúde Pública Universidade Federal de Goiás Goiânia Brazil

4. Laboratório de Micologia, Instituto Nacional de Infectologia Evandro Chagas Fundação Oswaldo Cruz (Fiocruz) Rio de Janeiro Brazil

Abstract

During the infectious process, pathogenic microorganisms must obtain nutrients from the host in order to survive and proliferate. These nutritional sources include the metallic nutrient copper. Despite its essentiality, copper in large amounts is toxic. Host defense mechanisms use high copper poisoning as a fungicidal strategy to control infection. Transcriptional analyses showed that yeast cultured in the presence of copper or inside macrophages (24 h) had elevated expression of CRP1, a copper efflux pump, suggesting that Histoplasma capsulatum could be exposed to a high copper environment in macrophages during the innate immune stage of infection. Accordingly, macrophages cultured in high copper are more efficient in controlling H. capsulatum growth. Also, silencing of ATP7a, a copper pump that promotes the copper influx in phagosomes, increases fungal survival in macrophages. The rich copper environment faced by the fungus is not dependent on IFN‐γ, since fungal CRP1 expression is induced in untreated macrophages. Appropriately, CRP1 knockdown fungal strains are more susceptible to macrophage control than wild‐type yeasts. Additionally, CRP1 silencing decreases fungal burden in mice during the phase of innate immune response (4‐day postinfection) and CRP1 is required for full virulence in a macrophage cell lines (J774 A.1 and RAW 264.7), as well as primary cells (BMDM). Thus, induction of fungal copper detoxifying genes during innate immunity and the attenuated virulence of CRP1‐knockdown yeasts suggest that H. capsulatum is exposed to a copper‐rich environment at early infection, but circumvents this condition to establish infection.

Funder

Conselho Nacional de Desenvolvimento Científico e Tecnológico

Fundação de Amparo à Pesquisa do Estado de Goiás

Publisher

Wiley

Subject

Cell Biology,Molecular Biology,Biochemistry

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