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Antigen density and applied force control enrichment of nanobody-expressing yeast cells in microfluidics.

Merlin SanicasRémy TorroLaurent LimozinPatrick Chames
Published in: Lab on a chip (2024)
In vitro display technologies such as yeast display have been instrumental in developing the selection of new antibodies, antibody fragments or nanobodies that bind to a specific target, with affinity towards the target being the main factor that influences selection outcome. However, the roles of mechanical forces are being increasingly recognized as a crucial factor in the regulation and activation of effector cell function. It would thus be of interest to isolate binders behaving optimally under the influence of mechanical forces. We developed a microfluidic assay allowing the selection of yeast displaying nanobodies through antigen-specific immobilization on a surface under controlled hydrodynamic flow. This approach enabled enrichment of model yeast mixtures using tunable antigen density and applied force. This new force-based selection method opens the possibility of selecting binders by relying on both their affinity and force resistance, with implications for the design of more efficient immunotherapeutics.
Keyphrases
  • single molecule
  • saccharomyces cerevisiae
  • cell wall
  • high throughput
  • induced apoptosis
  • cell cycle arrest
  • dendritic cells
  • endoplasmic reticulum stress
  • immune response
  • label free