Scientific Reports (Mar 2021)

Pharmacological targeting of host chaperones protects from pertussis toxin in vitro and in vivo

  • Katharina Ernst,
  • Ann-Katrin Mittler,
  • Veronika Winkelmann,
  • Carolin Kling,
  • Nina Eberhardt,
  • Anna Anastasia,
  • Michael Sonnabend,
  • Robin Lochbaum,
  • Jan Wirsching,
  • Moona Sakari,
  • Arto T. Pulliainen,
  • Ciaran Skerry,
  • Nicholas H. Carbonetti,
  • Manfred Frick,
  • Holger Barth

DOI
https://doi.org/10.1038/s41598-021-84817-2
Journal volume & issue
Vol. 11, no. 1
pp. 1 – 17

Abstract

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Abstract Whooping cough is caused by Bordetella pertussis that releases pertussis toxin (PT) which comprises enzyme A-subunit PTS1 and binding/transport B-subunit. After receptor-mediated endocytosis, PT reaches the endoplasmic reticulum from where unfolded PTS1 is transported to the cytosol. PTS1 ADP-ribosylates G-protein α-subunits resulting in increased cAMP signaling. Here, a role of target cell chaperones Hsp90, Hsp70, cyclophilins and FK506-binding proteins for cytosolic PTS1-uptake is demonstrated. PTS1 specifically and directly interacts with chaperones in vitro and in cells. Specific pharmacological chaperone inhibition protects CHO-K1, human primary airway basal cells and a fully differentiated airway epithelium from PT-intoxication by reducing intracellular PTS1-amounts without affecting cell binding or enzyme activity. PT is internalized by human airway epithelium secretory but not ciliated cells and leads to increase of apical surface liquid. Cyclophilin-inhibitors reduced leukocytosis in infant mouse model of pertussis, indicating their promising potential for developing novel therapeutic strategies against whooping cough.