Aspergillus fumigatus calcium-responsive transcription factors regulate cell wall architecture promoting stress tolerance, virulence and caspofungin resistance.

Patrícia Alves De Castro,Adriana Oliveira Manfiolli,Gustavo H Goldman,Fausto Almeida,Laure Nicolas Annick Ries,Lilian Pereira Silva,Gabriel Scalini De Souza,Giuseppe Palmisano,Neil Andrew Brown,Ana Cristina Colabardini,Marina Campos Rocha,Roberto Nascimento Silva,Flávio Vieira Loures,Iran Malavazi,Jéssica Chiaratto,Laura Mellado,Michael Bromley,Eliciane Cevolani Mattos,Gabriela Félix Persinoti

doi:10.1371/journal.pgen.1008551

Abstract

Aspergillus fumigatus causes invasive aspergillosis, the most common life-threatening fungal disease of immuno-compromised humans. The treatment of disseminated infections with antifungal drugs, including echinocandin cell wall biosynthesis inhibitors, is increasingly challenging due to the rise of drug-resistant pathogens. The fungal calcium responsive calcineurin-CrzA pathway influences cell morphology, cell wall composition, virulence, and echinocandin resistance. A screen of 395 A. fumigatus transcription factor mutants identified nine transcription factors important to calcium stress tolerance, including CrzA and ZipD. Here, comparative transcriptomics revealed CrzA and ZipD regulated the expression of shared and unique gene networks, suggesting they participate in both converged and distinct stress response mechanisms. CrzA and ZipD additively promoted calcium stress tolerance. However, ZipD also regulated cell wall organization, osmotic stress tolerance and echinocandin resistance. The absence of ZipD in A. fumigatus caused a significant virulence reduction in immunodeficient and immunocompetent mice. The ΔzipD mutant displayed altered cell wall organization and composition, while being more susceptible to macrophage killing and eliciting an increased pro-inflammatory cytokine response. A higher number of neutrophils, macrophages and activated macrophages were found in ΔzipD infected mice lungs. Collectively, this shows that ZipD-mediated regulation of the fungal cell wall contributes to the evasion of pro-inflammatory responses and tolerance of echinocandin antifungals, and in turn promoting virulence and complicating treatment options.

Highlights

Aspergillus fumigatus is a filamentous fungus that can cause disease in humans [1]
CrzA has been recognized as the sole calcium/calcineurin-dependent transcription factor (TF)
We identify nine TFs involved in the calcium/calcineurin metabolism, including a novel A. fumigatus calcium/calcineurin dependent TF named ZipD

Summary

Introduction

Depending on a patient’s immunological status, A. fumigatus can cause a distinct set of clinical disorders that extend from severe allergies to lethal disseminated infections [1]. Disseminated fungal infections are treated with antifungal drugs, including polyenes, azoles, and echinocandins [7]. Calcium is an essential secondary messenger and modulates the conformation of calciumbinding proteins, such as calmodulin, which activates calmodulin-dependent enzymes including the calcineurin phosphatase [10, 11]. Calcineurin regulates the activity of the Crz1p/CrzA transcription factor [12,13,14,15] with the phosphorylated form accumulating in the cell cytosol. In response to certain stimuli, which increase cytosolic calcium, calcineurin dephosphorylates Crz1p/CrzA leading to its re-localization to the nucleus. Crz1p/CrzA contains a C2H2 zinc finger motif that binds to a specific CDRE (calcineurin-dependent response element) at gene promoters, to direct calcium- and calcineurin-dependent gene expression [16]

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Results

Discussion

Conclusion