AI Article Synopsis

  • Candida glabrata is the second-most common cause of candidiasis in immunocompromised individuals, with a rising incidence largely due to its antifungal resistance and biofilm formation capabilities.
  • Research focused on the impact of the QDR2 gene on biofilm formation, comparing a mutant strain (C glabrata Δqdr2) with its wild-type counterpart.
  • Results showed that the Δqdr2 mutant had lower adhesion, higher susceptibility to fluconazole, reduced metabolic activity, and impaired growth under specific pH conditions, indicating that Qdr2p is crucial for effective biofilm formation and resistance in C glabrata.

Article Abstract

Candida glabrata represents the second-most frequent cause of candidiasis infections of the mucosa, bloodstream and genito-urinary tract in immunocompromised individuals. The incidence of C glabrata infection has increased significantly in the last two decades, mainly due to this species' abilities to resist various antifungal drugs and to form biofilms. We focused on the relationship between biofilm formation and the product of QDR2, a C glabrata member of the major facilitator superfamily (MFS) gene family, given that fungal biofilm formation limits drug penetration and is associated with persistent infection. The fungal cells in biofilms were compared between a C glabrata ∆qdr2 mutant and its wild-type strain. Cells were analysed for metabolism activity and drug susceptibility (using tetrazolium assay), adhesion activity, growth assay and intracellular pH (using flow cytometry). Compared to the wild type, the C glabrata ∆qdr2 showed lower adhesion activity and higher fluconazole susceptibility when assessed as a biofilm. The mutant also showed decreased metabolic activity during biofilm formation. Furthermore, the mutant grew more slowly under neutral-basic pH conditions. The qdr2 deletion in C glabrata resulted in an impaired ability to maintain pH homeostasis, which led in turn to a reduction of cell growth and of adherence to an artificial matrix. These results suggested that the Qdr2p function is needed for proper biofilm formation and biofilm maintenance in C glabrata as well as biofilm drug resistance towards fluconazole. Qdr2p may play an important role in C glabrata's ability to form biofilms on implanted medical devices in human bodies.

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http://dx.doi.org/10.1111/myc.13005DOI Listing

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