Macrocycle-stabilization of its interaction with 14-3-3 increases plasma membrane localization and activity of CFTR

Loes M. Stevers; Madita Wolter; Graeme W. Carlile; Dwight Macdonald; Luc Richard; Frank Gielkens; John W. Hanrahan; David Y. Thomas; Sai Kumar Chakka; Mark L. Peterson; Helmut Thomas; Luc Brunsveld; Christian Ottmann

Journal ArticleOPEN ACCESS

Macrocycle-stabilization of its interaction with 14-3-3 increases plasma membrane localization and activity of CFTR

Nature Communications (2022) 13(1)

DOI: 10.1038/s41467-022-31206-6

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Abstract

Impaired activity of the chloride channel CFTR is the cause of cystic fibrosis. 14-3-3 proteins have been shown to stabilize CFTR and increase its biogenesis and activity. Here, we report the identification and mechanism of action of a macrocycle stabilizing the 14-3-3/CFTR complex. This molecule rescues plasma membrane localization and chloride transport of F508del-CFTR and works additively with the CFTR pharmacological chaperone corrector lumacaftor (VX-809) and the triple combination Trikafta®. This macrocycle is a useful tool to study the CFTR/14-3-3 interaction and the potential of molecular glues in cystic fibrosis therapeutics.

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Stevers, L. M., Wolter, M., Carlile, G. W., Macdonald, D., Richard, L., Gielkens, F., … Ottmann, C. (2022). Macrocycle-stabilization of its interaction with 14-3-3 increases plasma membrane localization and activity of CFTR. Nature Communications, 13(1). https://doi.org/10.1038/s41467-022-31206-6

Macrocycle-stabilization of its interaction with 14-3-3 increases plasma membrane localization and activity of CFTR

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