| Literature DB >> 26041577 |
Emanuela Pesce1, Marta Bellotti2, Nara Liessi3, Sara Guariento4, Gianluca Damonte2, Elena Cichero4, Andrea Galatini5, Annalisa Salis6, Ambra Gianotti1, Nicoletta Pedemonte1, Olga Zegarra-Moran1, Paola Fossa4, Luis J V Galietta1, Enrico Millo7.
Abstract
The cystic fibrosis transmembrane conductance regulator (CFTR) is a chloride channel present in the membrane of epithelial cells. Mutations affecting the CFTR gene cause cystic fibrosis (CF), a multi-organ severe disease. The most common CF mutation, F508del, impairs the processing and activity (gating) of CFTR protein. Other mutations, like G551D, only cause a gating defect. Processing and gating defects can be targeted by small molecules called generically correctors and potentiators, respectively. Aminoarylthiazoles (AATs) represent an interesting class of compounds that includes molecules with dual activity, as correctors and potentiators. With the aim to improve the activity profile of AATs, we have now designed and synthesized a library of novel compounds in order to establish an initial SAR that may provide indications about the chemical groups that are beneficial or detrimental for rescue activity. The new compounds were tested as correctors and potentiators in CFBE41o-expressing F508del-CFTR using a functional assay. A dual active compound, AAT-4a, characterized by improved efficacy and marked synergy when combined with the corrector VX-809 has been identified. Moreover, by computational methods, a possible binding site for AATs in nucleotide binding domain NBD1 has been detected. These results will direct the synthesis of new analogues with possibly improved activity.Entities:
Keywords: AminoArylthiazole; CFTR; Corrector; Cystic fibrosis; Docking; SAR
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Year: 2015 PMID: 26041577 DOI: 10.1016/j.ejmech.2015.05.030
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514