Candida albicans is an opportunistic fungal pathogen. It is the fourth leading cause of nosocomial infections and can endanger immunocompromised patients. Candida has the ability to form biofilms on plastic medical devices, such as catheters and central nervous system shunts. Two clinical isolate series were profiled using a number of phenotyping assays comprising in vivo, ex vivo, and in vitro tests. These tests shed light on host-pathogen relations as well as offer potential information useful in the treatment of these infections. Fluconazole, an antifungal, is the first line of treatment for fungal infections. The incidence of fluconazole-resistant infections is increasing annually, and there are not many other drugs available to treat infections. In 2013, Fazly et al. discovered the drug Filastatin, which prevents adhesion and filamentation of Candida albicans. In our study, two screens were performed to identify the target of Filastatin. Because there is no complete knockout library for Candida, an available, partial knockout library was screened. This library is enriched for transcription factors. We screened for regulators of biological pathways that may be important for adhesion and filamentation in Candida albicans, to identify potential Filastatin targets. The iron-uptake pathway was chosen as the focus for the remainder of this study.

Creator

• Harwood, Catherine

Contributeurs

• Gegear, Robert J.
• Rao, Reeta Prusty
• Srinivasan, Jagan

Degree

• MS

Unit

• Biology & Biotechnology

Publisher

• Worcester Polytechnic Institute

Language

• English

Identifier

• etd-043015-092345

Mot-clé

• iron uptake
• filastatin
• Candida albicans
• animal models

Advisor

• Rao, Reeta Prusty

Committee

• Gegear, Robert J.
• Srinivasan, Jagan

Defense date

• 2015-04-24

Year

• 2015

Date created

• 2015-04-30

Resource type

• Thesis

Rights statement

• In Copyright

Dernière modification

• 2021-02-02