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Biphasic zinc compartmentalisation in a human fungal pathogen

by Skrahina, Volha , Alawfi, Bader , Costa, Anna C. B. P. , Ballou, Elizabeth R. , Urban, Constantin F. , Yellagunda, Sujan , Wilson, Duncan , Crawford, Aaron C. , Lehtovirta-Morley, Laura E. , Anderson, Andrew , Alsarraf, Mohammad , Hube, Bernhard , Alamir, Omran , Niemiec, Maria J.

in Adaptation, Physiological / Animals / Antimicrobial Cationic Peptides - genetics / Antimicrobial Cationic Peptides - metabolism / Biocompatibility / Bioinformatics / Biology / Biology and Life Sciences / Calgranulin B - genetics / Calgranulin B - metabolism / Candida albicans / Candida albicans - genetics / Candida albicans - metabolism / Candida albicans - pathogenicity / Candidiasis, Invasive - metabolism / Candidiasis, Invasive - microbiology / Carrier Proteins - genetics / Carrier Proteins - metabolism / Cation Transport Proteins - genetics / Cation Transport Proteins - metabolism / Cell Compartmentation / Chelation / Clonal deletion / Colonization / Councils / Cryptococcus neoformans / Deletion mutant / Female / Fungal Proteins - genetics / Fungal Proteins - metabolism / Fungi / Gene Deletion / Gene mutation / Genes, Fungal / Genetic aspects / Health aspects / Homeostasis / Host-Pathogen Interactions - genetics / Host-Pathogen Interactions - physiology / Humans / Hydrogen-Ion Concentration / Immunity / Imports / Infections / Iron / Kidneys / Leukocyte L1 Antigen Complex - genetics / Leukocyte L1 Antigen Complex - metabolism / Liver / Male / Manganese / Medical research / Medicine and Health Sciences / Mice / Mice, Inbred C57BL / Mice, Knockout / Micronutrients / Mutants / Natural products / Neutrophils / Pathogens / pH effects / Physical Sciences / Pollution tolerance / Proteins / Research and Analysis Methods / Saccharomyces cerevisiae / Sepsis / Supervision / Virulence / Virulence - genetics / Virulence - physiology / Zinc / Zinc (Nutrient) / Zinc - metabolism / Zinc - toxicity

2018

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Biphasic zinc compartmentalisation in a human fungal pathogen

2018

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2018

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Journal Article

Biphasic zinc compartmentalisation in a human fungal pathogen

Skrahina, Volha,

Alawfi, Bader,

Costa, Anna C. B. P.,

Ballou, Elizabeth R.,

Urban, Constantin F.,

Yellagunda, Sujan,

Wilson, Duncan,

Crawford, Aaron C.,

Lehtovirta-Morley, Laura E.,

Anderson, Andrew,

Alsarraf, Mohammad,

Hube, Bernhard,

Alamir, Omran,

Niemiec, Maria J.

2018

Overview

Nutritional immunity describes the host-driven manipulation of essential micronutrients, including iron, zinc and manganese. To withstand nutritional immunity and proliferate within their hosts, pathogenic microbes must express efficient micronutrient uptake and homeostatic systems. Here we have elucidated the pathway of cellular zinc assimilation in the major human fungal pathogen Candida albicans. Bioinformatics analysis identified nine putative zinc transporters: four cytoplasmic-import Zip proteins (Zrt1, Zrt2, Zrt3 and orf19.5428) and five cytoplasmic-export ZnT proteins (orf19.1536/Zrc1, orf19.3874, orf19.3769, orf19.3132 and orf19.52). Only Zrt1 and Zrt2 are predicted to localise to the plasma membrane and here we demonstrate that Zrt2 is essential for C. albicans zinc uptake and growth at acidic pH. In contrast, ZRT1 expression was found to be highly pH-dependent and could support growth of the ZRT2-null strain at pH 7 and above. This regulatory paradigm is analogous to the distantly related pathogenic mould, Aspergillus fumigatus, suggesting that pH-adaptation of zinc transport may be conserved in fungi and we propose that environmental pH has shaped the evolution of zinc import systems in fungi. Deletion of C. albicans ZRT2 reduced kidney fungal burden in wild type, but not in mice lacking the zinc-chelating antimicrobial protein calprotectin. Inhibition of zrt2Δ growth by neutrophil extracellular traps was calprotectin-dependent. This suggests that, within the kidney, C. albicans growth is determined by pathogen-Zrt2 and host-calprotectin. As well as serving as an essential micronutrient, zinc can also be highly toxic and we show that C. albicans deals with this potential threat by rapidly compartmentalising zinc within vesicular stores called zincosomes. In order to understand mechanistically how this process occurs, we created deletion mutants of all five ZnT-type transporters in C. albicans. Here we show that, unlike in Saccharomyces cerevisiae, C. albicans Zrc1 mediates zinc tolerance via zincosomal zinc compartmentalisation. This novel transporter was also essential for virulence and liver colonisation in vivo. In summary, we show that zinc homeostasis in a major human fungal pathogen is a multi-stage process initiated by Zrt1/Zrt2-cellular import, followed by Zrc1-dependent intracellular compartmentalisation.

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Publisher

Public Library of Science,Public Library of Science (PLoS)

Subject

Adaptation, Physiological

/ Animals

/ Antimicrobial Cationic Peptides - genetics

/ Antimicrobial Cationic Peptides - metabolism

/ Biocompatibility

/ Bioinformatics

/ Biology