Cryptococcus gattii in North American Pacific Northwest: whole-population genome analysis provides insights into species evolution and dispersal

The emergence of distinct populations of Cryptococcus gattii in the temperate North American Pacific Northwest (PNW) was surprising, as this species was previously thought to be confined to tropical and semitropical regions. Beyond a new habitat niche, the dominant emergent population displayed incr...

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Published inmBio Vol. 5; no. 4; p. e01464
Main Authors Engelthaler, David M, Hicks, Nathan D, Gillece, John D, Roe, Chandler C, Schupp, James M, Driebe, Elizabeth M, Gilgado, Felix, Carriconde, Fabian, Trilles, Luciana, Firacative, Carolina, Ngamskulrungroj, Popchai, Castañeda, Elizabeth, Lazera, Marcia dos Santos, Melhem, Marcia S C, Pérez-Bercoff, Asa, Huttley, Gavin, Sorrell, Tania C, Voelz, Kerstin, May, Robin C, Fisher, Matthew C, Thompson, 3rd, George R, Lockhart, Shawn R, Keim, Paul, Meyer, Wieland
Format Journal Article
LanguageEnglish
Published United States American Society of Microbiology 15.07.2014
American Society for Microbiology
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Summary:The emergence of distinct populations of Cryptococcus gattii in the temperate North American Pacific Northwest (PNW) was surprising, as this species was previously thought to be confined to tropical and semitropical regions. Beyond a new habitat niche, the dominant emergent population displayed increased virulence and caused primary pulmonary disease, as opposed to the predominantly neurologic disease seen previously elsewhere. Whole-genome sequencing was performed on 118 C. gattii isolates, including the PNW subtypes and the global diversity of molecular type VGII, to better ascertain the natural source and genomic adaptations leading to the emergence of infection in the PNW. Overall, the VGII population was highly diverse, demonstrating large numbers of mutational and recombinational events; however, the three dominant subtypes from the PNW were of low diversity and were completely clonal. Although strains of VGII were found on at least five continents, all genetic subpopulations were represented or were most closely related to strains from South America. The phylogenetic data are consistent with multiple dispersal events from South America to North America and elsewhere. Numerous gene content differences were identified between the emergent clones and other VGII lineages, including genes potentially related to habitat adaptation, virulence, and pathology. Evidence was also found for possible gene introgression from Cryptococcus neoformans var. grubii that is rarely seen in global C. gattii but that was present in all PNW populations. These findings provide greater understanding of C. gattii evolution in North America and support extensive evolution in, and dispersal from, South America. Importance: Cryptococcus gattii emerged in the temperate North American Pacific Northwest (PNW) in the late 1990s. Beyond a new environmental niche, these emergent populations displayed increased virulence and resulted in a different pattern of clinical disease. In particular, severe pulmonary infections predominated in contrast to presentation with neurologic disease as seen previously elsewhere. We employed population-level whole-genome sequencing and analysis to explore the genetic relationships and gene content of the PNW C. gattii populations. We provide evidence that the PNW strains originated from South America and identified numerous genes potentially related to habitat adaptation, virulence expression, and clinical presentation. Characterization of these genetic features may lead to improved diagnostics and therapies for such fungal infections. The data indicate that there were multiple recent introductions of C. gattii into the PNW. Public health vigilance is warranted for emergence in regions where C. gattii is not thought to be endemic.
Bibliography:Editor Arturo Casadevall, Albert Einstein College of Medicine
This article is a direct contribution from a member of the American Academy of Microbiology.
D.M.E. and N.D.H. contributed equally to this article.
ISSN:2161-2129
2150-7511
DOI:10.1128/mBio.01464-14