Affiliation:
1. Department of Microbiology and Immunology, University of California San Francisco, San Francisco, California, USA
2. Howard Hughes Medical Institute, Chevy Chase, Maryland, USA
Abstract
ABSTRACT
Histoplasma capsulatum
is a fungal pathogen that infects both healthy and immunocompromised hosts. In regions where it is endemic,
H. capsulatum
grows in the soil and causes respiratory and systemic disease when inhaled by humans. An interesting aspect of
H. capsulatum
biology is that it adopts specialized developmental programs in response to its environment. In the soil, it grows as filamentous chains of cells (mycelia) that produce asexual spores (conidia). When the soil is disrupted, conidia aerosolize and are inhaled by mammalian hosts. Inside a host, conidia germinate into yeast-form cells that colonize immune cells and cause disease. Despite the ability of conidia to initiate infection and disease, they have not been explored on a molecular level. We developed methods to purify
H. capsulatum
conidia, and we show here that these cells germinate into filaments at room temperature and into yeast-form cells at 37°C. Conidia internalized by macrophages germinate into the yeast form and proliferate within macrophages, ultimately lysing the host cells. Similarly, infection of mice with purified conidia is sufficient to establish infection and yield viable yeast-form cells
in vivo
. To characterize conidia on a molecular level, we performed whole-genome expression profiling of conidia, yeast, and mycelia from two highly divergent
H. capsulatum
strains. In parallel, we used homology and protein domain analysis to manually annotate the predicted genes of both strains. Analyses of the resultant data defined sets of transcripts that reflect the unique molecular states of
H. capsulatum
conidia, yeast, and mycelia.
Publisher
American Society for Microbiology
Subject
Molecular Biology,General Medicine,Microbiology
Cited by
46 articles.
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