ADAM8 expression in invasive breast cancer promotes tumor dissemination and metastasis

The transmembrane metalloprotease-disintegrin ADAM8 mediates cell adhesion and shedding of ligands, receptors and extracellular matrix components. Here, we report that ADAM8 is abundantly expressed in breast tumors and derived metastases compared to normal tissue, especially in triple-negative breas...

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Autores principales: Romagnoli, Mathilde, Mineva, Nora D, Polmear, Michael, Conrad, Catharina, Srinivasan, Srimathi, Loussouarn, Delphine, Barillé-Nion, Sophie, Georgakoudi, Irene, Dagg, Áine, McDermott, Enda W, Duffy, Michael J, McGowan, Patricia M, Schlomann, Uwe, Parsons, Maddy, Bartsch, Jörg W, Sonenshein, Gail E
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Blackwell Publishing Ltd 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3927960/
https://www.ncbi.nlm.nih.gov/pubmed/24375628
http://dx.doi.org/10.1002/emmm.201303373
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author Romagnoli, Mathilde
Mineva, Nora D
Polmear, Michael
Conrad, Catharina
Srinivasan, Srimathi
Loussouarn, Delphine
Barillé-Nion, Sophie
Georgakoudi, Irene
Dagg, Áine
McDermott, Enda W
Duffy, Michael J
McGowan, Patricia M
Schlomann, Uwe
Parsons, Maddy
Bartsch, Jörg W
Sonenshein, Gail E
author_facet Romagnoli, Mathilde
Mineva, Nora D
Polmear, Michael
Conrad, Catharina
Srinivasan, Srimathi
Loussouarn, Delphine
Barillé-Nion, Sophie
Georgakoudi, Irene
Dagg, Áine
McDermott, Enda W
Duffy, Michael J
McGowan, Patricia M
Schlomann, Uwe
Parsons, Maddy
Bartsch, Jörg W
Sonenshein, Gail E
author_sort Romagnoli, Mathilde
collection PubMed
description The transmembrane metalloprotease-disintegrin ADAM8 mediates cell adhesion and shedding of ligands, receptors and extracellular matrix components. Here, we report that ADAM8 is abundantly expressed in breast tumors and derived metastases compared to normal tissue, especially in triple-negative breast cancers (TNBCs). Furthermore, high ADAM8 levels predicted poor patient outcome. Consistently, ADAM8 promoted an aggressive phenotype of TNBC cells in culture. In a mouse orthotopic model, tumors derived from TNBC cells with ADAM8 knockdown failed to grow beyond a palpable size and displayed poor vascularization. Circulating tumor cells and brain metastases were also significantly reduced. Mechanistically, ADAM8 stimulated both angiogenesis through release of VEGF-A and transendothelial cell migration via β1-integrin activation. In vivo, treatment with an anti-ADAM8 antibody from the time of cell inoculation reduced primary tumor burden and metastases. Furthermore, antibody treatment of established tumors profoundly decreased metastases in a resection model. As a non-essential protein under physiological conditions, ADAM8 represents a promising novel target for treatment of TNBCs, which currently lack targeted therapies and frequently progress with fatal dissemination. Subject Category Cancer
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spelling pubmed-39279602014-02-28 ADAM8 expression in invasive breast cancer promotes tumor dissemination and metastasis Romagnoli, Mathilde Mineva, Nora D Polmear, Michael Conrad, Catharina Srinivasan, Srimathi Loussouarn, Delphine Barillé-Nion, Sophie Georgakoudi, Irene Dagg, Áine McDermott, Enda W Duffy, Michael J McGowan, Patricia M Schlomann, Uwe Parsons, Maddy Bartsch, Jörg W Sonenshein, Gail E EMBO Mol Med Research Article The transmembrane metalloprotease-disintegrin ADAM8 mediates cell adhesion and shedding of ligands, receptors and extracellular matrix components. Here, we report that ADAM8 is abundantly expressed in breast tumors and derived metastases compared to normal tissue, especially in triple-negative breast cancers (TNBCs). Furthermore, high ADAM8 levels predicted poor patient outcome. Consistently, ADAM8 promoted an aggressive phenotype of TNBC cells in culture. In a mouse orthotopic model, tumors derived from TNBC cells with ADAM8 knockdown failed to grow beyond a palpable size and displayed poor vascularization. Circulating tumor cells and brain metastases were also significantly reduced. Mechanistically, ADAM8 stimulated both angiogenesis through release of VEGF-A and transendothelial cell migration via β1-integrin activation. In vivo, treatment with an anti-ADAM8 antibody from the time of cell inoculation reduced primary tumor burden and metastases. Furthermore, antibody treatment of established tumors profoundly decreased metastases in a resection model. As a non-essential protein under physiological conditions, ADAM8 represents a promising novel target for treatment of TNBCs, which currently lack targeted therapies and frequently progress with fatal dissemination. Subject Category Cancer Blackwell Publishing Ltd 2014-02 2013-12-27 /pmc/articles/PMC3927960/ /pubmed/24375628 http://dx.doi.org/10.1002/emmm.201303373 Text en © 2013 The Authors. http://creativecommons.org/licenses/by/3.0/ This is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Romagnoli, Mathilde
Mineva, Nora D
Polmear, Michael
Conrad, Catharina
Srinivasan, Srimathi
Loussouarn, Delphine
Barillé-Nion, Sophie
Georgakoudi, Irene
Dagg, Áine
McDermott, Enda W
Duffy, Michael J
McGowan, Patricia M
Schlomann, Uwe
Parsons, Maddy
Bartsch, Jörg W
Sonenshein, Gail E
ADAM8 expression in invasive breast cancer promotes tumor dissemination and metastasis
title ADAM8 expression in invasive breast cancer promotes tumor dissemination and metastasis
title_full ADAM8 expression in invasive breast cancer promotes tumor dissemination and metastasis
title_fullStr ADAM8 expression in invasive breast cancer promotes tumor dissemination and metastasis
title_full_unstemmed ADAM8 expression in invasive breast cancer promotes tumor dissemination and metastasis
title_short ADAM8 expression in invasive breast cancer promotes tumor dissemination and metastasis
title_sort adam8 expression in invasive breast cancer promotes tumor dissemination and metastasis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3927960/
https://www.ncbi.nlm.nih.gov/pubmed/24375628
http://dx.doi.org/10.1002/emmm.201303373
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