Integrins regulate hERG1 dynamics by girdin-dependent Gαi3: signaling and modeling in cancer cells

The hERG1 potassium channel is aberrantly over expressed in tumors and regulates the cancer cell response to integrin-dependent adhesion. We unravel a novel signaling pathway by which integrin engagement by the ECM protein fibronectin promotes hERG1 translocation to the plasma membrane and its assoc...

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Autores principales: Duranti, Claudia, Iorio, Jessica, Bagni, Giacomo, Chioccioli Altadonna, Ginevra, Fillion, Thibault, Lulli, Matteo, D’Alessandro, Franco Nicolas, Montalbano, Alberto, Lastraioli, Elena, Fanelli, Duccio, Coppola, Stefano, Schmidt, Thomas, Piazza, Francesco, Becchetti, Andrea, Arcangeli, Annarosa
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Life Science Alliance LLC 2023
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10624597/
https://www.ncbi.nlm.nih.gov/pubmed/37923359
http://dx.doi.org/10.26508/lsa.202302135
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author Duranti, Claudia
Iorio, Jessica
Bagni, Giacomo
Chioccioli Altadonna, Ginevra
Fillion, Thibault
Lulli, Matteo
D’Alessandro, Franco Nicolas
Montalbano, Alberto
Lastraioli, Elena
Fanelli, Duccio
Coppola, Stefano
Schmidt, Thomas
Piazza, Francesco
Becchetti, Andrea
Arcangeli, Annarosa
author_facet Duranti, Claudia
Iorio, Jessica
Bagni, Giacomo
Chioccioli Altadonna, Ginevra
Fillion, Thibault
Lulli, Matteo
D’Alessandro, Franco Nicolas
Montalbano, Alberto
Lastraioli, Elena
Fanelli, Duccio
Coppola, Stefano
Schmidt, Thomas
Piazza, Francesco
Becchetti, Andrea
Arcangeli, Annarosa
author_sort Duranti, Claudia
collection PubMed
description The hERG1 potassium channel is aberrantly over expressed in tumors and regulates the cancer cell response to integrin-dependent adhesion. We unravel a novel signaling pathway by which integrin engagement by the ECM protein fibronectin promotes hERG1 translocation to the plasma membrane and its association with β1 integrins, by activating girdin-dependent Gαi3 proteins and protein kinase B (Akt). By sequestering hERG1, β1 integrins make it avoid Rab5-mediated endocytosis, where unbound channels are degraded. The cycle of hERG1 expression determines the resting potential (V(rest)) oscillations and drives the cortical f-actin dynamics and thus cell motility. To interpret the slow biphasic kinetics of hERG1/β1 integrin interplay, we developed a mathematical model based on a generic balanced inactivation–like module. Integrin-mediated cell adhesion triggers two contrary responses: a rapid stimulation of hERG1/β1 complex formation, followed by a slow inhibition which restores the initial condition. The protracted hERG1/β1 integrin cycle determines the slow time course and cyclic behavior of cell migration in cancer cells.
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spelling pubmed-106245972023-11-05 Integrins regulate hERG1 dynamics by girdin-dependent Gαi3: signaling and modeling in cancer cells Duranti, Claudia Iorio, Jessica Bagni, Giacomo Chioccioli Altadonna, Ginevra Fillion, Thibault Lulli, Matteo D’Alessandro, Franco Nicolas Montalbano, Alberto Lastraioli, Elena Fanelli, Duccio Coppola, Stefano Schmidt, Thomas Piazza, Francesco Becchetti, Andrea Arcangeli, Annarosa Life Sci Alliance Research Articles The hERG1 potassium channel is aberrantly over expressed in tumors and regulates the cancer cell response to integrin-dependent adhesion. We unravel a novel signaling pathway by which integrin engagement by the ECM protein fibronectin promotes hERG1 translocation to the plasma membrane and its association with β1 integrins, by activating girdin-dependent Gαi3 proteins and protein kinase B (Akt). By sequestering hERG1, β1 integrins make it avoid Rab5-mediated endocytosis, where unbound channels are degraded. The cycle of hERG1 expression determines the resting potential (V(rest)) oscillations and drives the cortical f-actin dynamics and thus cell motility. To interpret the slow biphasic kinetics of hERG1/β1 integrin interplay, we developed a mathematical model based on a generic balanced inactivation–like module. Integrin-mediated cell adhesion triggers two contrary responses: a rapid stimulation of hERG1/β1 complex formation, followed by a slow inhibition which restores the initial condition. The protracted hERG1/β1 integrin cycle determines the slow time course and cyclic behavior of cell migration in cancer cells. Life Science Alliance LLC 2023-11-03 /pmc/articles/PMC10624597/ /pubmed/37923359 http://dx.doi.org/10.26508/lsa.202302135 Text en © 2023 Duranti et al. https://creativecommons.org/licenses/by/4.0/This article is available under a Creative Commons License (Attribution 4.0 International, as described at https://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Articles
Duranti, Claudia
Iorio, Jessica
Bagni, Giacomo
Chioccioli Altadonna, Ginevra
Fillion, Thibault
Lulli, Matteo
D’Alessandro, Franco Nicolas
Montalbano, Alberto
Lastraioli, Elena
Fanelli, Duccio
Coppola, Stefano
Schmidt, Thomas
Piazza, Francesco
Becchetti, Andrea
Arcangeli, Annarosa
Integrins regulate hERG1 dynamics by girdin-dependent Gαi3: signaling and modeling in cancer cells
title Integrins regulate hERG1 dynamics by girdin-dependent Gαi3: signaling and modeling in cancer cells
title_full Integrins regulate hERG1 dynamics by girdin-dependent Gαi3: signaling and modeling in cancer cells
title_fullStr Integrins regulate hERG1 dynamics by girdin-dependent Gαi3: signaling and modeling in cancer cells
title_full_unstemmed Integrins regulate hERG1 dynamics by girdin-dependent Gαi3: signaling and modeling in cancer cells
title_short Integrins regulate hERG1 dynamics by girdin-dependent Gαi3: signaling and modeling in cancer cells
title_sort integrins regulate herg1 dynamics by girdin-dependent gαi3: signaling and modeling in cancer cells
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10624597/
https://www.ncbi.nlm.nih.gov/pubmed/37923359
http://dx.doi.org/10.26508/lsa.202302135
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