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A uniquely efficacious type of CFTR corrector with complementary mode of action

SCIENCE ADVANCES. 2024-03; 
Valentina Marchesin,?Lucile Monnier,?Peter Blattmann,?Florent Chevillard,?Christine Kuntz,?Camille Forny,?Judith Kamper,?Rolf Studer,?Alexandre Bossu,?Eric A Ertel,?Oliver Nayler,?Christine Brotschi,?Jodi T Williams,?John Gatfield
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PCR Cloning and Subcloning Samples were mixed with LDS sample buffer (Invitrogen), resolved by SDS-PAGE on 4 to 12% Novex bis-tris precast gels (Thermo Fisher Scientific), and analyzed by Western blotting using a wet transfer method (GenScript) and polyvinylidene difluoride membranes (Life Technologies). Get A Quote

摘要

Three distinct pharmacological corrector types (I, II, III) with different binding sites and additive behavior only partially rescue the F508del-cystic fibrosis transmembrane conductance regulator (CFTR) folding and trafficking defect observed in cystic fibrosis. We describe uniquely effective, macrocyclic CFTR correctors that were additive to the known corrector types, exerting a complementary “type IV” corrector mechanism. Macrocycles achieved wild-type–like folding efficiency of F508del-CFTR at the endoplasmic reticulum and normalized CFTR currents in reconstituted patient-derived bronchial epithelium. Using photo-activatable macrocycles, docking studies and site-directed mutagenesis a highly probable ... More

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