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Evaluation of a systems biology approach to identify pharmacological correctors of the mutant CFTR chloride channel

Authors :
Diego Carrella
Francesco Sirci
Olga Zegarra-Moran
Giulia Gorrieri
Luis J. V. Galietta
Emanuela Pesce
Francesco Napolitano
Valeria Tomati
Emanuela Caci
Diego di Bernardo
Pesce, Emanuela
Gorrieri, Giulia
Sirci, Francesco
Napolitano, Francesco
Carrella, Diego
Caci, Emanuela
Tomati, Valeria
Zegarra Moran, Olga
DI BERNARDO, Diego
Galietta, Luis J. V.
Source :
Journal of cystic fibrosis : official journal of the European Cystic Fibrosis Society. 15(4)
Publication Year :
2015

Abstract

Background Mistrafficking of CFTR protein caused by F508del, the most frequent mutation in cystic fibrosis (CF), can be corrected by cell incubation at low temperature, an effect that may be mediated by altered expression of proteostasis genes. Methods To identify small molecules mimicking low temperature, we compared gene expression profiles of cells kept at 27°C with those previously generated from more than 1300 compounds. The resulting candidates were tested with a functional assay on a bronchial epithelial cell line. Results We found that anti-inflammatory glucocorticoids, such as mometasone, budesonide, and fluticasone, increased mutant CFTR function. However, this activity was not confirmed in primary bronchial epithelial cells. Actually, glucocorticoids enhanced Na + absorption, an effect that could further impair mucociliary clearance in CF airways. Conclusions Our results suggest that rescue of F508del-CFTR by low temperature cannot be easily mimicked by small molecules and that compounds with closer transcriptional and functional effects need to be found.

Details

ISSN :
18735010
Volume :
15
Issue :
4
Database :
OpenAIRE
Journal :
Journal of cystic fibrosis : official journal of the European Cystic Fibrosis Society
Accession number :
edsair.doi.dedup.....045301d03aa475799ca0d7f7a3400572