Molecular Mechanism of Action of Trimethylangelicin Derivatives as CFTR Modulators

The psoralen-related compound, 4,6,4′-trimethylangelicin (TMA) potentiates the cAMP/PKA-dependent activation of WT-CFTR and rescues F508del-CFTR-dependent chloride secretion in both primary and secondary airway cells homozygous for the F508del mutation. We recently demonstrated that TMA, like lumaca...

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Autores principales: Laselva, Onofrio, Marzaro, Giovanni, Vaccarin, Christian, Lampronti, Ilaria, Tamanini, Anna, Lippi, Giuseppe, Gambari, Roberto, Cabrini, Giulio, Bear, Christine E., Chilin, Adriana, Dechecchi, Maria C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6039571/
https://www.ncbi.nlm.nih.gov/pubmed/30022950
http://dx.doi.org/10.3389/fphar.2018.00719
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author Laselva, Onofrio
Marzaro, Giovanni
Vaccarin, Christian
Lampronti, Ilaria
Tamanini, Anna
Lippi, Giuseppe
Gambari, Roberto
Cabrini, Giulio
Bear, Christine E.
Chilin, Adriana
Dechecchi, Maria C.
author_facet Laselva, Onofrio
Marzaro, Giovanni
Vaccarin, Christian
Lampronti, Ilaria
Tamanini, Anna
Lippi, Giuseppe
Gambari, Roberto
Cabrini, Giulio
Bear, Christine E.
Chilin, Adriana
Dechecchi, Maria C.
author_sort Laselva, Onofrio
collection PubMed
description The psoralen-related compound, 4,6,4′-trimethylangelicin (TMA) potentiates the cAMP/PKA-dependent activation of WT-CFTR and rescues F508del-CFTR-dependent chloride secretion in both primary and secondary airway cells homozygous for the F508del mutation. We recently demonstrated that TMA, like lumacaftor (VX-809), stabilizes the first membrane-spanning domain (MSD1) and enhances the interface between NBD1 and ICL4 (MSD2). TMA also demonstrated anti-inflammatory properties, via reduction of IL-8 expression, thus making TMA a promising agent for treatment of cystic fibrosis. Unfortunately, TMA was also found to display potential phototoxicity and mutagenicity, despite the fact that photo-reactivity is absent when the compound is not directly irradiated with UVA light. Due to concerns about these toxic effects, new TMA analogs, characterized by identical or better activity profiles and minimized or reduced side effects, were synthesized by modifying specific structural features on the TMA scaffold, thus generating compounds with no mutagenicity and phototoxicity. Among these compounds, we found TMA analogs which maintained the potentiation activity of CFTR in FRT-YFP-G551D cells. Nanomolar concentrations of these analogs significantly rescued F508del CFTR-dependent chloride efflux in FRT-YFP-F508del, HEK-293 and CF bronchial epithelial cells. We then investigated the ability of TMA analogs to enhance the stable expression of varying CFTR truncation mutants in HEK-293 cells, with the aim of studying the mechanism of their corrector activity. Not surprisingly, MSD1 was the smallest domain stabilized by TMA analogs, as previously observed for TMA. Moreover, we found that TMA analogs were not effective on F508del-CFTR protein which was already stabilized by a second-site mutation at the NBD1-ICL4 interface. Altogether, our findings demonstrate that these TMA analogs mediate correction by modifying MSD1 and indirectly stabilizing the interface between NBD1 and CL4.
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spelling pubmed-60395712018-07-18 Molecular Mechanism of Action of Trimethylangelicin Derivatives as CFTR Modulators Laselva, Onofrio Marzaro, Giovanni Vaccarin, Christian Lampronti, Ilaria Tamanini, Anna Lippi, Giuseppe Gambari, Roberto Cabrini, Giulio Bear, Christine E. Chilin, Adriana Dechecchi, Maria C. Front Pharmacol Pharmacology The psoralen-related compound, 4,6,4′-trimethylangelicin (TMA) potentiates the cAMP/PKA-dependent activation of WT-CFTR and rescues F508del-CFTR-dependent chloride secretion in both primary and secondary airway cells homozygous for the F508del mutation. We recently demonstrated that TMA, like lumacaftor (VX-809), stabilizes the first membrane-spanning domain (MSD1) and enhances the interface between NBD1 and ICL4 (MSD2). TMA also demonstrated anti-inflammatory properties, via reduction of IL-8 expression, thus making TMA a promising agent for treatment of cystic fibrosis. Unfortunately, TMA was also found to display potential phototoxicity and mutagenicity, despite the fact that photo-reactivity is absent when the compound is not directly irradiated with UVA light. Due to concerns about these toxic effects, new TMA analogs, characterized by identical or better activity profiles and minimized or reduced side effects, were synthesized by modifying specific structural features on the TMA scaffold, thus generating compounds with no mutagenicity and phototoxicity. Among these compounds, we found TMA analogs which maintained the potentiation activity of CFTR in FRT-YFP-G551D cells. Nanomolar concentrations of these analogs significantly rescued F508del CFTR-dependent chloride efflux in FRT-YFP-F508del, HEK-293 and CF bronchial epithelial cells. We then investigated the ability of TMA analogs to enhance the stable expression of varying CFTR truncation mutants in HEK-293 cells, with the aim of studying the mechanism of their corrector activity. Not surprisingly, MSD1 was the smallest domain stabilized by TMA analogs, as previously observed for TMA. Moreover, we found that TMA analogs were not effective on F508del-CFTR protein which was already stabilized by a second-site mutation at the NBD1-ICL4 interface. Altogether, our findings demonstrate that these TMA analogs mediate correction by modifying MSD1 and indirectly stabilizing the interface between NBD1 and CL4. Frontiers Media S.A. 2018-07-04 /pmc/articles/PMC6039571/ /pubmed/30022950 http://dx.doi.org/10.3389/fphar.2018.00719 Text en Copyright © 2018 Laselva, Marzaro, Vaccarin, Lampronti, Tamanini, Lippi, Gambari, Cabrini, Bear, Chilin and Dechecchi. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Laselva, Onofrio
Marzaro, Giovanni
Vaccarin, Christian
Lampronti, Ilaria
Tamanini, Anna
Lippi, Giuseppe
Gambari, Roberto
Cabrini, Giulio
Bear, Christine E.
Chilin, Adriana
Dechecchi, Maria C.
Molecular Mechanism of Action of Trimethylangelicin Derivatives as CFTR Modulators
title Molecular Mechanism of Action of Trimethylangelicin Derivatives as CFTR Modulators
title_full Molecular Mechanism of Action of Trimethylangelicin Derivatives as CFTR Modulators
title_fullStr Molecular Mechanism of Action of Trimethylangelicin Derivatives as CFTR Modulators
title_full_unstemmed Molecular Mechanism of Action of Trimethylangelicin Derivatives as CFTR Modulators
title_short Molecular Mechanism of Action of Trimethylangelicin Derivatives as CFTR Modulators
title_sort molecular mechanism of action of trimethylangelicin derivatives as cftr modulators
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6039571/
https://www.ncbi.nlm.nih.gov/pubmed/30022950
http://dx.doi.org/10.3389/fphar.2018.00719
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