Abstract

Oral thrush, a mucosal biofilm infection, continues to afflict an unacceptably high percentage of immunocompromised individuals, particularly neonates and patients on immunosuppressive medications. Although C. albicans is the primary etiologic pathogen, the microbial ecology of this infection is complex since it contains members of the endogenous bacterial flora. Candida forms mixed biofilms with streptococci in the oral cavities of humans but the role of these biofilms during the course of mucosa-associated or invasive infections is unknown. In the proposed work C. albicans and S. oralis will be used as model organisms to study the mucosal disease-promoting interactions of the non-pathogenic oral bacterial flora with opportunistic fungi that have established virulence, such as C. albicans. Our studies rely upon a systematic and comprehensive approach to characterize both host- and pathogen-mediated aspects of the pathogenesis of mixed opportunistic mucosal infections. We hypothesize that enhanced proinflammatory host responses and increased Candida virulence mediate a pathogenic synergy of these microorganisms in the oral and esophageal mucosa.
In aim I we will characterize the influence of streptococci on the TLR2/4-mediated host response to mixed infection and test the hypothesis that the exaggerated proinflammatory and neutrophilic response to mixed Candida-streptococcal biofilms leads to increased pathology.
In aim II we will examine mechanisms of mixed microbial community assembly and virulence. The role of streptococcal glucosyltransferases, major enzymes contributing to the extracellular slime that promotes biofilms, will be examined. In C. albicans we will identify the transcription factor(s) tht control dual community assembly. We will also test the hypothesis that S. oralis increases the virulence of C. albicans by modulating several Rim101-dependent virulence genes, important in oral mucosal invasion, using a mouse oral co-infection model. An understanding of the effects of oral streptococci on Candida virulence and the mucosal inflammatory response will provide important novel insights into the pathogenesis of fungal infection within the oral and esophageal host niche. More importantly, the discovery of a synergistic role for oral bacteria in pathogenesis may have important clinical implications in the treatment of oral thrush which is currently based solely on antifungals.

Public Health Relevance

Oral thrush (also known as candidiasis) is still the most prevalent form of infection in patients with weakened or immature immune systems such as HIV+ children, neonates and patients with malignancies. We propose that certain oral bacteria cooperate with the principal fungal species responsible for this infection, Candida albicans, to trigger inflammatory mucosal lesions that are a cause for severe morbidity in millions of individuals worldwide. Defining the mechanism of microbial synergy in mucosal polymicrobial infections is important, because these infections are notoriously resistant to antimicrobials and thus there is an urgent need for the development of new prevention and treatment strategies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Project (R01)
Project #
5R01DE013986-14
Application #
9256456
Study Section
Oral, Dental and Craniofacial Sciences Study Section (ODCS)
Program Officer
Chander, Preethi
Project Start
2000-09-29
Project End
2019-04-30
Budget Start
2017-05-01
Budget End
2018-04-30
Support Year
14
Fiscal Year
2017
Total Cost
$398,750
Indirect Cost
$148,750

  Institution

Name
University of Connecticut
Department
Dentistry
Type
Schools of Dentistry
DUNS #
022254226
City
Farmington
State
CT
Country
United States
Zip Code
06030

  Publications

Sobue, T; Bertolini, M; Thompson, A et al. (2018) Chemotherapy-induced oral mucositis and associated infections in a novel organotypic model. Mol Oral Microbiol 33:212-223
Bertolini, M; Sobue, T; Thompson, A et al. (2017) Chemotherapy Induces Oral Mucositis in Mice Without Additional Noxious Stimuli. Transl Oncol 10:612-620
Xu, Hongbin; Sobue, Takanori; Bertolini, Martinna et al. (2017) S. oralis activates the Efg1 filamentation pathway in C. albicans to promote cross-kingdom interactions and mucosal biofilms. Virulence 8:1602-1617
Xu, Hongbin; Sobue, Takanori; Bertolini, Martinna et al. (2016) Streptococcus oralis and Candida albicans Synergistically Activate ?-Calpain to Degrade E-cadherin From Oral Epithelial Junctions. J Infect Dis 214:925-34
Sobue, Takanori; Diaz, Patricia; Xu, Hongbin et al. (2016) Experimental Models of C. albicans-Streptococcal Co-infection. Methods Mol Biol 1356:137-52
Xu, H; Dongari-Bagtzoglou, A (2015) Shaping the oral mycobiota: interactions of opportunistic fungi with oral bacteria and the host. Curr Opin Microbiol 26:65-70
Bertolini, M M; Xu, H; Sobue, T et al. (2015) Candida-streptococcal mucosal biofilms display distinct structural and virulence characteristics depending on growth conditions and hyphal morphotypes. Mol Oral Microbiol 30:307-22
Xu, H; Jenkinson, H F; Dongari-Bagtzoglou, A (2014) Innocent until proven guilty: mechanisms and roles of Streptococcus-Candida interactions in oral health and disease. Mol Oral Microbiol 29:99-116
Diaz, Patricia I; Strausbaugh, Linda D; Dongari-Bagtzoglou, Anna (2014) Fungal-bacterial interactions and their relevance to oral health: linking the clinic and the bench. Front Cell Infect Microbiol 4:101
Ricker, Austin; Vickerman, Margaret; Dongari-Bagtzoglou, Anna (2014) Streptococcus gordonii glucosyltransferase promotes biofilm interactions with Candida albicans. J Oral Microbiol 6:

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