Science and Research

The potentiator ivacaftor is essential for pharmacological restoration of F508del-CFTR function and mucociliary clearance in cystic fibrosis

Pharmacological rescue of F508del-CFTR by the triple combination CFTR modulator therapy elexacaftor/tezacaftor/ivacaftor (ETI) leads to unprecedented clinical benefits in patients with cystic fibrosis (CF). However, previous studies in CF primary human airway epithelial cultures demonstrated that chronic treatment with the potentiator ivacaftor can render the F508del protein unstable, thus limiting restoration of CFTR chloride channel function. Even so, quantitative studies of this unwanted effect of ivacaftor on F508del channel function with dependency on cell culture conditions remain limited, and the impact of chronic ivacaftor exposure on restoration of mucociliary clearance that is impaired in patients with CF has not been studied. In patient-derived primary nasal epithelial cultures, we found that different culture conditions (UNC-ALI medium vs. PneumaCult medium) have profound effects on ETI-mediated restoration of F508del-CFTR function. Chronic treatment with ivacaftor as part of ETI triple therapy limited the rescue of F508del-CFTR chloride channel function when CF nasal epithelial cultures were grown in UNC-ALI medium but not in PneumaCult medium. In PneumaCult medium, both chronic and acute addition of ivacaftor as part of ETI treatment led to constitutive CFTR-mediated chloride secretion in the absence of exogenous cAMP-dependent stimulation. This constitutive CFTR-mediated chloride secretion was essential to improve viscoelastic properties of the mucus layer and to restore mucociliary transport on CF nasal epithelial cultures. Furthermore, nasal potential difference measurements in patients with CF showed that ETI restored constitutive F508del-CFTR activity in vivo. These results demonstrate that ivacaftor as a component of ETI therapy is essential to restore mucociliary clearance and suggest that this effect is facilitated by its constitutive activation of F508del channels following their folding correction in patients with CF.

  • Balázs, A.
  • Rubil, T.
  • Wong, C. K.
  • Berger, J.
  • Drescher, M.
  • Seidel, K.
  • Stahl, M.
  • Graeber, S. Y.
  • Mall, M. A.

Keywords

  • *Cystic Fibrosis Transmembrane Conductance Regulator/genetics/metabolism/drug
  • effects
  • *Quinolones/pharmacology/therapeutic use
  • *Aminophenols/pharmacology/therapeutic use
  • Humans
  • *Cystic Fibrosis/drug therapy/genetics/metabolism
  • *Mucociliary Clearance/drug effects
  • Animals
  • Benzodioxoles/pharmacology
  • Cells, Cultured
  • Nasal Mucosa/drug effects/metabolism
  • Chloride Channel Agonists/pharmacology
  • Epithelial Cells/drug effects/metabolism
  • Pyrazoles/pharmacology
  • Female
  • Male
  • Indoles/pharmacology
  • Cell biology
  • Chloride channels
  • Genetic diseases
  • Pulmonology
Publication details
DOI: 10.1172/jci.insight.187951
Journal: JCI Insight
Number: 10
Work Type: Original
Location: Assoziierter Partner
Disease Area: CFBE
Partner / Member: BIH
Access-Number: 40261705


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