Single Amino Acid Substitutions in the Chemotactic Sequence of Urokinase Receptor Modulate Cell Migration and Invasion

The receptor for urokinase-type plasminogen activator (uPAR) plays an important role in controlling cell migration. uPAR binds urokinase and vitronectin extracellular ligands, and signals in complex with transmembrane receptors such as Formyl-peptide Receptors (FPR)s and integrins. Previous work fro...

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Autores principales: Bifulco, Katia, Longanesi-Cattani, Immacolata, Franco, Paola, Pavone, Vincenzo, Mugione, Pietro, Di Carluccio, Gioconda, Masucci, Maria Teresa, Arra, Claudio, Pirozzi, Giuseppe, Stoppelli, Maria Patrizia, Carriero, Maria Vincenza
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3458052/
https://www.ncbi.nlm.nih.gov/pubmed/23049759
http://dx.doi.org/10.1371/journal.pone.0044806
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author Bifulco, Katia
Longanesi-Cattani, Immacolata
Franco, Paola
Pavone, Vincenzo
Mugione, Pietro
Di Carluccio, Gioconda
Masucci, Maria Teresa
Arra, Claudio
Pirozzi, Giuseppe
Stoppelli, Maria Patrizia
Carriero, Maria Vincenza
author_facet Bifulco, Katia
Longanesi-Cattani, Immacolata
Franco, Paola
Pavone, Vincenzo
Mugione, Pietro
Di Carluccio, Gioconda
Masucci, Maria Teresa
Arra, Claudio
Pirozzi, Giuseppe
Stoppelli, Maria Patrizia
Carriero, Maria Vincenza
author_sort Bifulco, Katia
collection PubMed
description The receptor for urokinase-type plasminogen activator (uPAR) plays an important role in controlling cell migration. uPAR binds urokinase and vitronectin extracellular ligands, and signals in complex with transmembrane receptors such as Formyl-peptide Receptors (FPR)s and integrins. Previous work from this laboratory has shown that synthetic peptides, corresponding to the uPAR(88–92) chemotactic sequence, when carrying the S90P or S90E substitutions, up- or down-regulate cell migration, respectively. To gain mechanistic insights into these opposite cell responses, the functional consequences of S90P and S90E mutations in full-length uPAR were evaluated. First, (HEK)-293 embryonic kidney cells expressing uPAR(S90P) exhibit enhanced FPR activation, increased random and directional cell migration, long-lasting Akt phosphorylation, and increased adhesion to vitronectin, as well as uPAR/vitronectin receptor association. In contrast, the S90E substitution prevents agonist-triggered FPR activation and internalization, decreases binding and adhesion to vitronectin, and inhibits uPAR/vitronectin receptor association. Also, 293/uPAR(S90P) cells appear quite elongated and their cytoskeleton well organized, whereas 293/uPAR(S90E) cells assume a large flattened morphology, with random orientation of actin filaments. Interestingly, when HT1080 cells co-express wild type uPAR with uPAR S90E, the latter behaves as a dominant-negative, impairing uPAR-mediated signaling and reducing cell wound repair as well as lung metastasis in nude mice. In contrast, signaling, wound repair and in vivo lung metastasis of HT1080 cells bearing wild type uPAR are enhanced when they co-express uPAR(S90P). In conclusion, our findings indicate that Ser(90) is a critical residue for uPAR signaling and that the S90P and S90E exert opposite effects on uPAR activities. These findings may be accommodated in a molecular model, in which uPAR(S90E) and uPAR(S90P) are forced into inactive and active forms, respectively, suggesting important implications for the development of novel drugs targeting uPAR function.
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spelling pubmed-34580522012-10-03 Single Amino Acid Substitutions in the Chemotactic Sequence of Urokinase Receptor Modulate Cell Migration and Invasion Bifulco, Katia Longanesi-Cattani, Immacolata Franco, Paola Pavone, Vincenzo Mugione, Pietro Di Carluccio, Gioconda Masucci, Maria Teresa Arra, Claudio Pirozzi, Giuseppe Stoppelli, Maria Patrizia Carriero, Maria Vincenza PLoS One Research Article The receptor for urokinase-type plasminogen activator (uPAR) plays an important role in controlling cell migration. uPAR binds urokinase and vitronectin extracellular ligands, and signals in complex with transmembrane receptors such as Formyl-peptide Receptors (FPR)s and integrins. Previous work from this laboratory has shown that synthetic peptides, corresponding to the uPAR(88–92) chemotactic sequence, when carrying the S90P or S90E substitutions, up- or down-regulate cell migration, respectively. To gain mechanistic insights into these opposite cell responses, the functional consequences of S90P and S90E mutations in full-length uPAR were evaluated. First, (HEK)-293 embryonic kidney cells expressing uPAR(S90P) exhibit enhanced FPR activation, increased random and directional cell migration, long-lasting Akt phosphorylation, and increased adhesion to vitronectin, as well as uPAR/vitronectin receptor association. In contrast, the S90E substitution prevents agonist-triggered FPR activation and internalization, decreases binding and adhesion to vitronectin, and inhibits uPAR/vitronectin receptor association. Also, 293/uPAR(S90P) cells appear quite elongated and their cytoskeleton well organized, whereas 293/uPAR(S90E) cells assume a large flattened morphology, with random orientation of actin filaments. Interestingly, when HT1080 cells co-express wild type uPAR with uPAR S90E, the latter behaves as a dominant-negative, impairing uPAR-mediated signaling and reducing cell wound repair as well as lung metastasis in nude mice. In contrast, signaling, wound repair and in vivo lung metastasis of HT1080 cells bearing wild type uPAR are enhanced when they co-express uPAR(S90P). In conclusion, our findings indicate that Ser(90) is a critical residue for uPAR signaling and that the S90P and S90E exert opposite effects on uPAR activities. These findings may be accommodated in a molecular model, in which uPAR(S90E) and uPAR(S90P) are forced into inactive and active forms, respectively, suggesting important implications for the development of novel drugs targeting uPAR function. Public Library of Science 2012-09-25 /pmc/articles/PMC3458052/ /pubmed/23049759 http://dx.doi.org/10.1371/journal.pone.0044806 Text en © 2012 Bifulco 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
Bifulco, Katia
Longanesi-Cattani, Immacolata
Franco, Paola
Pavone, Vincenzo
Mugione, Pietro
Di Carluccio, Gioconda
Masucci, Maria Teresa
Arra, Claudio
Pirozzi, Giuseppe
Stoppelli, Maria Patrizia
Carriero, Maria Vincenza
Single Amino Acid Substitutions in the Chemotactic Sequence of Urokinase Receptor Modulate Cell Migration and Invasion
title Single Amino Acid Substitutions in the Chemotactic Sequence of Urokinase Receptor Modulate Cell Migration and Invasion
title_full Single Amino Acid Substitutions in the Chemotactic Sequence of Urokinase Receptor Modulate Cell Migration and Invasion
title_fullStr Single Amino Acid Substitutions in the Chemotactic Sequence of Urokinase Receptor Modulate Cell Migration and Invasion
title_full_unstemmed Single Amino Acid Substitutions in the Chemotactic Sequence of Urokinase Receptor Modulate Cell Migration and Invasion
title_short Single Amino Acid Substitutions in the Chemotactic Sequence of Urokinase Receptor Modulate Cell Migration and Invasion
title_sort single amino acid substitutions in the chemotactic sequence of urokinase receptor modulate cell migration and invasion
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3458052/
https://www.ncbi.nlm.nih.gov/pubmed/23049759
http://dx.doi.org/10.1371/journal.pone.0044806
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