Abstract

In the United States, as many as 10% of hospitalized patients develop a nosocomial infection, estimated to involve more than 2 million patients (and 58,000 deaths), and to cost more than $4.5 billion annually. Candida species represent the 6th most common nosocomial pathogen overall, and the 4th most common cause of nosocomial bloodstream infections. Mortality from systemic candidiasis ranges from 63% to 85% in untreated patients and from 33% to 54% in those who receive appropriate antifungal therapy. Patients at highest risk include immunosuppressed patients, trauma patients, and postsurgical patients. The intestinal tract is believed to be the major colonizing habitat, and the source of most Candida infection. C. albicans accounts for 60% to 80% of all Candida isolates and C. albicans is the most virulent species. C. albicans is eucaryotic and diploid, and it is not possible to construct isogenic mutants using techniques designed for procaryotic bacteria. However, using the """"""""Ura-blaster"""""""" method, it has recently become possible to construct isogenic strains of C. albicans that differ from a parent strain by disruption of a single gene; the gene INT1 has been associated with epithelial adhesion, morphogenesis (switching from yeast to hyphal forms), and virulence. In this proposal, well characterized wild-type and mutant strains of C. albicans (carrying two, one, or zero copies of INT1) are used to clarify the pathogenic significance of C. albicans adherence and morphogenesis, emphasizing the oral route of infection in clinically relevant mouse models of surgery and trauma, where experimental variables include antibiotic therapy, parenteral endotoxin, and hypoxia. Relevant in vitro cell culture systems (HT-29 and Caco-2 enterocytes) are also used where more defined conditions can be used to correlate the degree of C. albicans filamentation (production of germ tubes, pseudohyphae, true hyphae) with the degree of adherence, internalization, intracellular survival, and paracellular and transcellular migration. Results from in vitro cell culture systems are correlated with results from in vivo models. The working hypothesis is: Morphologic switching in C. albicans, that is conversion from yeast to hyphal forms, plays a key role in C. albicans adherence and invasion, and thus plays a key role in C. albicans pathogenesis and virulence. Thus, the overall aim is to clarify the relevance of adhesion and morphogenesis in C. albicans pathogenesis. The long term goal is to use this information to target novel treatment regimens to decrease the costly morbidity and mortality associated with systemic candidiasis in surgical patients and trauma patients.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM059221-04
Application #
6519995
Study Section
Special Emphasis Panel (ZRG1-SSS-W (15))
Program Officer
Somers, Scott D
Project Start
1999-06-01
Project End
2003-11-30
Budget Start
2002-06-01
Budget End
2003-11-30
Support Year
4
Fiscal Year
2002
Total Cost
$201,765
Indirect Cost

  Institution

Name
University of Minnesota Twin Cities
Department
Pathology
Type
Schools of Medicine
DUNS #
168559177
City
Minneapolis
State
MN
Country
United States
Zip Code
55455

  Publications

Hess, Donavon J; Henry-Stanley, Michelle J; Bendel, Catherine M et al. (2009) Escherichia coli and TNF-alpha modulate macrophage phagocytosis of Candida glabrata. J Surg Res 155:217-24
Henry-Stanley, Michelle J; Wells, Carol L (2009) Polyethylene glycol influences microbial interactions with intestinal epithelium. Shock 31:390-6
Brand, Alexandra; Vacharaksa, Anjalee; Bendel, Catherine et al. (2008) An internal polarity landmark is important for externally induced hyphal behaviors in Candida albicans. Eukaryot Cell 7:712-20
Wells, Carol L; Johnson, Mary-Alice; Henry-Stanley, Michelle J et al. (2007) Candida glabrata colonizes but does not often disseminate from the mouse caecum. J Med Microbiol 56:688-93
Erlandsen, Stanley L; Kristich, Christopher J; Dunny, Gary M et al. (2004) High-resolution visualization of the microbial glycocalyx with low-voltage scanning electron microscopy: dependence on cationic dyes. J Histochem Cytochem 52:1427-35
Wells, Carol L; Hess, Donavon J; Erlandsen, Stanley L (2004) Impact of the indigenous flora in animal models of shock and sepsis. Shock 22:562-8
Henry-Stanley, Michelle J; Garni, Robb M; Wells, Carol L (2004) Adaptation of FUN-1 and Calcofluor white stains to assess the ability of viable and nonviable yeast to adhere to and be internalized by cultured mammalian cells. J Microbiol Methods 59:289-92
Henry-Stanley, Michelle J; Hess, Donavon J; Erickson, Elizabeth A et al. (2003) Effect of lipopolysaccharide on virulence of intestinal candida albicans. J Surg Res 113:42-9
Kim, Adam S; Garni, Robb M; Henry-Stanley, Michelle J et al. (2003) Hypoxia and extraintestinal dissemination of Candida albicans yeast forms. Shock 19:257-62
Bendel, Catherine M; Hess, Donavon J; Garni, Robb M et al. (2003) Comparative virulence of Candida albicans yeast and filamentous forms in orally and intravenously inoculated mice. Crit Care Med 31:501-7

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