| Literature DB >> 29272749 |
Nara Liessi1, Elena Cichero2, Emanuela Pesce3, Maria Arkel4, Annalisa Salis5, Valeria Tomati3, Matteo Paccagnella4, Gianluca Damonte1, Bruno Tasso2, Luis J V Galietta3, Nicoletta Pedemonte3, Paola Fossa6, Enrico Millo7.
Abstract
The most common CF mutation, F508del, impairs the processing and gating of CFTR protein. This deletion results in the improper folding of the protein and its degradation before it reaches the plasma membrane of epithelial cells. Present correctors, like VX809 only induce a partial rescue of the mutant protein. Our previous studies reported a class of compounds, called aminoarylthiazoles (AATs), featuring an interesting activity as correctors. Some of them show additive effect with VX809 indicating a different mechanism of action. In an attempt to construct more interesting molecules, it was thought to generate chemically hybrid compounds, blending a portion of VX809 merged to the thiazole scaffold. This approach was guided by the development of QSAR analyses, which were performed based on the F508del correctors so far disclosed in the literature. This strategy was aimed at exploring the key requirements turning in the corrector ability of the collected derivatives and allowed us to derive a predictive model guiding for the synthesis of novel hybrids as promising correctors. The new molecules were tested in functional and biochemical assays on bronchial CFBE41o-cells expressing F508del-CFTR showing a promising corrector activity.Entities:
Keywords: Aminoarylthiazole; CFTR; Corrector; Cystic fibrosis; QSAR; VX809
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Year: 2017 PMID: 29272749 DOI: 10.1016/j.ejmech.2017.12.030
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514