4.8 Article

Single-cell force spectroscopy of the medically important Staphylococcus epidermidis-Candida albicans interaction

Journal

NANOSCALE
Volume 5, Issue 22, Pages 10894-10900

Publisher

ROYAL SOC CHEMISTRY
DOI: 10.1039/c3nr03272h

Keywords

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Funding

  1. National Foundation for Scientific Research (FNRS)
  2. Universite catholique de Louvain (Fonds Speciaux de Recherche)
  3. Region Wallonne
  4. Federal Office for Scientific, Technical and Cultural Affairs (Interuniversity Poles of Attraction Programme)
  5. Research Department of the Communaute francaise de Belgique (Concerted Research Action)
  6. Flemish Science Foundation (FWO)
  7. KU Leuven
  8. Interuniversity Attraction Poles Programme
  9. Belgian Science Policy Office (IAP) [P7/28]
  10. NIH [R01 GM 098616]

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Despite the clinical importance of bacterial-fungal interactions, their molecular details are poorly understood. A hallmark of such medically important interspecies associations is the interaction between the two nosocomial pathogens Staphylococcus aureus and Candida albicans, which can lead to mixed biofilm-associated infections with enhanced antibiotic resistance. Here, we use single-cell force spectroscopy (SCFS) to quantify the forces engaged in bacterial-fungal co-adhesion, focusing on the poorly investigated S. epidermidis-C. albicans interaction. Force curves recorded between single bacterial and fungal germ tubes showed large adhesion forces (similar to 5 nN) with extended rupture lengths (up to 500 nm). By contrast, bacteria poorly adhered to yeast cells, emphasizing the important role of the yeast-to-hyphae transition in mediating adhesion to bacterial cells. Analysis of mutant strains altered in cell wall composition allowed us to distinguish the main fungal components involved in adhesion, i.e. Als proteins and O-mannosylations. We suggest that the measured co-adhesion forces are involved in the formation of mixed biofilms, thus possibly as well in promoting polymicrobial infections. In the future, we anticipate that this SCFS platform will be used in nanomedicine to decipher the molecular mechanisms of a wide variety of pathogen-pathogen interactions and may help in designing novel anti-adhesion agents.

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