Affiliation:
1. Department of Microbiology and Immunology, University of Texas Health Science Center at San Antonio, 7703 Floyd Curl Drive, MC 7758, San Antonio, Texas 78229-3900
Abstract
ABSTRACT
The ability of
Candida albicans
, the most common human fungal pathogen, to transition from yeast to hyphae is essential for pathogenicity. While a variety of transcription factors important for filamentation have been identified and characterized, links between transcriptional regulators of
C. albicans
morphogenesis and molecular mechanisms that drive hyphal growth are not well defined. We have previously observed that constitutive expression of
UME6
, which encodes a filament-specific transcriptional regulator, is sufficient to direct hyphal growth in the absence of filament-inducing conditions. Here we show that
HGC1
, encoding a cyclin-related protein necessary for hyphal growth under filament-inducing conditions, is specifically important for agar invasion, hyphal extension, and formation of true septa in response to constitutive
UME6
expression under non-filament-inducing conditions.
HGC1
-dependent inactivation of Rga2, a Cdc42 GTPase activating protein (GAP), also appears to be important for these processes. In response to filament-inducing conditions,
HGC1
is induced prior to
UME6
although
UME6
controls the level and duration of
HGC1
expression, which are likely to be important for hyphal extension. Interestingly, an epistasis analysis suggests that
UME6
and
HGC1
play distinct roles during early filament formation. These findings establish a link between a key regulator of filamentation and a downstream mechanism important for hyphal formation. In addition, this study demonstrates that a strain expressing constitutive high levels of
UME6
provides a powerful strategy to specifically dissect downstream mechanisms important for hyphal development in the absence of complex filament-inducing conditions.
Publisher
American Society for Microbiology
Subject
Molecular Biology,General Medicine,Microbiology
Cited by
59 articles.
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