Targeting Integrin-Dependent Adhesion and Signaling with 3-Arylquinoline and 3-Aryl-2-Quinolone Derivatives: A new Class of Integrin Antagonists

We previously reported the anti-migratory function of 3-aryl-2-quinolone derivatives, chemically close to flavonoids (Joseph et al., 2002). Herein we show that 3-arylquinoline or 3-aryl-2-quinolone derivatives disrupt cell adhesion in a dose dependent and reversible manner yet antagonized by artific...

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Autores principales: Fiorucci, Sandrine, Lin, Xiaochen, Sadoul, Karin, Fournet, Guy, Bouvard, Daniel, Vinogradova, Olga, Joseph, Benoît, Block, Marc R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4624933/
https://www.ncbi.nlm.nih.gov/pubmed/26509443
http://dx.doi.org/10.1371/journal.pone.0141205
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author Fiorucci, Sandrine
Lin, Xiaochen
Sadoul, Karin
Fournet, Guy
Bouvard, Daniel
Vinogradova, Olga
Joseph, Benoît
Block, Marc R.
author_facet Fiorucci, Sandrine
Lin, Xiaochen
Sadoul, Karin
Fournet, Guy
Bouvard, Daniel
Vinogradova, Olga
Joseph, Benoît
Block, Marc R.
author_sort Fiorucci, Sandrine
collection PubMed
description We previously reported the anti-migratory function of 3-aryl-2-quinolone derivatives, chemically close to flavonoids (Joseph et al., 2002). Herein we show that 3-arylquinoline or 3-aryl-2-quinolone derivatives disrupt cell adhesion in a dose dependent and reversible manner yet antagonized by artificial integrin activation such as manganese. Relying on this anti-adhesive activity, a Structure-Activity Relationship (SAR) study was established on 20 different compounds to throw the bases of future optimization strategies. Active drugs efficiently inhibit platelet spreading, aggregation, and clot retraction, processes that rely on α(llb)β(3) integrin activation and clustering. In vitro these derivatives interfere with β(3) cytoplasmic tail interaction with kindlin-2 in pulldown assays albeit little effect was observed with pure proteins suggesting that the drugs may block an alternative integrin activation process that may not be directly related to kindlin recruitment. Ex vivo, these drugs blunt integrin signaling assayed using focal adhesion kinase auto-phosphorylation as a read-out. Hence, 3-arylquinoline and 3-aryl-2-quinolone series are a novel class of integrin activation and signaling antagonists.
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spelling pubmed-46249332015-11-06 Targeting Integrin-Dependent Adhesion and Signaling with 3-Arylquinoline and 3-Aryl-2-Quinolone Derivatives: A new Class of Integrin Antagonists Fiorucci, Sandrine Lin, Xiaochen Sadoul, Karin Fournet, Guy Bouvard, Daniel Vinogradova, Olga Joseph, Benoît Block, Marc R. PLoS One Research Article We previously reported the anti-migratory function of 3-aryl-2-quinolone derivatives, chemically close to flavonoids (Joseph et al., 2002). Herein we show that 3-arylquinoline or 3-aryl-2-quinolone derivatives disrupt cell adhesion in a dose dependent and reversible manner yet antagonized by artificial integrin activation such as manganese. Relying on this anti-adhesive activity, a Structure-Activity Relationship (SAR) study was established on 20 different compounds to throw the bases of future optimization strategies. Active drugs efficiently inhibit platelet spreading, aggregation, and clot retraction, processes that rely on α(llb)β(3) integrin activation and clustering. In vitro these derivatives interfere with β(3) cytoplasmic tail interaction with kindlin-2 in pulldown assays albeit little effect was observed with pure proteins suggesting that the drugs may block an alternative integrin activation process that may not be directly related to kindlin recruitment. Ex vivo, these drugs blunt integrin signaling assayed using focal adhesion kinase auto-phosphorylation as a read-out. Hence, 3-arylquinoline and 3-aryl-2-quinolone series are a novel class of integrin activation and signaling antagonists. Public Library of Science 2015-10-28 /pmc/articles/PMC4624933/ /pubmed/26509443 http://dx.doi.org/10.1371/journal.pone.0141205 Text en © 2015 Fiorucci et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Fiorucci, Sandrine
Lin, Xiaochen
Sadoul, Karin
Fournet, Guy
Bouvard, Daniel
Vinogradova, Olga
Joseph, Benoît
Block, Marc R.
Targeting Integrin-Dependent Adhesion and Signaling with 3-Arylquinoline and 3-Aryl-2-Quinolone Derivatives: A new Class of Integrin Antagonists
title Targeting Integrin-Dependent Adhesion and Signaling with 3-Arylquinoline and 3-Aryl-2-Quinolone Derivatives: A new Class of Integrin Antagonists
title_full Targeting Integrin-Dependent Adhesion and Signaling with 3-Arylquinoline and 3-Aryl-2-Quinolone Derivatives: A new Class of Integrin Antagonists
title_fullStr Targeting Integrin-Dependent Adhesion and Signaling with 3-Arylquinoline and 3-Aryl-2-Quinolone Derivatives: A new Class of Integrin Antagonists
title_full_unstemmed Targeting Integrin-Dependent Adhesion and Signaling with 3-Arylquinoline and 3-Aryl-2-Quinolone Derivatives: A new Class of Integrin Antagonists
title_short Targeting Integrin-Dependent Adhesion and Signaling with 3-Arylquinoline and 3-Aryl-2-Quinolone Derivatives: A new Class of Integrin Antagonists
title_sort targeting integrin-dependent adhesion and signaling with 3-arylquinoline and 3-aryl-2-quinolone derivatives: a new class of integrin antagonists
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4624933/
https://www.ncbi.nlm.nih.gov/pubmed/26509443
http://dx.doi.org/10.1371/journal.pone.0141205
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