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Physiologically relevant alternative carbon sources modulate biofilm formation, cell wall architecture, and the stress and antifungal resistance of candida glabrata

International Journal of Molecular Sciences, ISSN: 1422-0067, Vol: 20, Issue: 13
2019
  • 34
    Citations
  • 0
    Usage
  • 56
    Captures
  • 1
    Mentions
  • 140
    Social Media
Metric Options:   Counts1 Year3 Year

Metrics Details

  • Citations
    34
  • Captures
    56
  • Mentions
    1
    • Blog Mentions
      1
      • Blog
        1
  • Social Media
    140
    • Shares, Likes & Comments
      140
      • Facebook
        140

Most Recent Blog

IJMS, Vol. 20, Pages 3172: Physiologically Relevant Alternative Carbon Sources Modulate Biofilm Formation, Cell Wall Architecture, and the Stress and Antifungal Resistance of Candida glabrata

IJMS, Vol. 20, Pages 3172: Physiologically Relevant Alternative Carbon Sources Modulate Biofilm Formation, Cell Wall Architecture, and the Stress and Antifungal Resistance of Candida glabrata

Article Description

Flexibility in carbon metabolism is pivotal for the survival and propagation of many human fungal pathogens within host niches. Indeed, flexible carbon assimilation enhances pathogenicity and affects the immunogenicity of Candida albicans. Over the last decade, Candida glabrata has emerged as one of the most common and problematic causes of invasive candidiasis. Despite this, the links between carbon metabolism, fitness, and pathogenicity in C. glabrata are largely unexplored. Therefore, this study has investigated the impact of alternative carbon metabolism on the fitness and pathogenic attributes of C. glabrata. We confirm our previous observation that growth on carbon sources other than glucose, namely acetate, lactate, ethanol, or oleate, attenuates both the planktonic and biofilm growth of C. glabrata, but that biofilms are not significantly affected by growth on glycerol. We extend this by showing that C. glabrata cells grown on these alternative carbon sources undergo cell wall remodeling, which reduces the thickness of their β-glucan and chitin inner layer while increasing their outer mannan layer. Furthermore, alternative carbon sources modulated the oxidative stress resistance of C. glabrata as well as the resistance of C. glabrata to an antifungal drug. In short, key fitness and pathogenic attributes of C. glabrata are shown to be dependent on carbon source. This reaffirms the perspective that the nature of the carbon sources available within specific host niches is crucial for C. glabrata pathogenicity during infection.

Bibliographic Details

Chew, Shu Yih; Ho, Kok Lian; Cheah, Yoke Kqueen; Sandai, Doblin; Brown, Alistair J P; Than, Leslie Thian Lung

MDPI AG

Chemical Engineering; Biochemistry, Genetics and Molecular Biology; Chemistry; Computer Science

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