Affiliation:
1. Department of Chemical Engineering, Texas A&M University, College Station, Texas, USA
Abstract
ABSTRACT
Candida
is a member of the normal human microbiota and often resides on mucosal surfaces such as the oral cavity or the gastrointestinal tract. In addition to their commensality,
Candida
species can opportunistically become pathogenic if the host microbiota is disrupted or if the host immune system becomes compromised. An important factor for
Candida
pathogenesis is its ability to form biofilm communities. The two most medically important species—
Candida albicans
and
Candida glabrata
—are often coisolated from infection sites, suggesting the importance of
Candida
coculture biofilms. In this work, we report that biofilm formation of the coculture population depends on the relative ratio of starting cell concentrations of
C. albicans
and
C. glabrata
. When using a starting ratio of
C. albicans
to
C. glabrata
of 1:3, ∼6.5- and ∼2.5-fold increases in biofilm biomass were observed relative to those of a
C. albicans
monoculture and a
C. albicans
/
C. glabrata
ratio of 1:1, respectively. Confocal microscopy analysis revealed the heterogeneity and complex structures composed of long
C. albicans
hyphae and
C. glabrata
cell clusters in the coculture biofilms, and reverse transcription-quantitative PCR (qRT-PCR) studies showed increases in the relative expression of the
HWP1
and
ALS3
adhesion genes in the
C. albicans
/
C. glabrata
1:3 biofilm compared to that in the
C. albicans
monoculture biofilm. Additionally, only the 1:3
C. albicans
/
C. glabrata
biofilm demonstrated an increased resistance to the antifungal drug caspofungin. Overall, the results suggest that interspecific interactions between these two fungal pathogens increase biofilm formation and virulence-related gene expression in a coculture composition-dependent manner.
IMPORTANCE
Candida albicans
and
Candida glabrata
are often coisolated during infection, and the occurrence of coisolation increases with increasing inflammation, suggesting possible synergistic interactions between the two
Candida
species in pathogenesis. During the course of an infection, the prevalence of each
Candida
species may change over time due to differences in metabolism and in the resistance of each species to antifungal therapies. Therefore, it is necessary to understand the dynamics between
C. albicans
and
C. glabrata
in coculture to develop better therapeutic strategies against
Candida
infections. Existing
in vitro
work has focused on understanding how an equal-part culture of
C. albicans
and
C. glabrata
impacts biofilm formation and pathogenesis. What is not understood, and what is investigated in this work, is how the composition of
Candida
species in coculture impacts overall biofilm formation, virulence gene expression, and the therapeutic treatment of biofilms.
Funder
National Science Foundation
Publisher
American Society for Microbiology
Subject
Ecology,Applied Microbiology and Biotechnology,Food Science,Biotechnology
Cited by
27 articles.
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