Compound genetically engineered mouse models of cancer reveal dual targeting of ALK1 and endoglin as a synergistic opportunity to impinge on angiogenic TGF-β signaling

Angiogenesis occurs early in tumor development, sustains primary tumor growth and provides a route for metastatic escape. The TGF-β family receptors modulate angiogenesis via endothelial-cell specific pathways. Here we investigate the interaction of two such receptors, ALK1 and endoglin, in pancreat...

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Autores principales: Eleftheriou, Nikolas M., Sjölund, Jonas, Bocci, Matteo, Cortez, Eliane, Lee, Se-Jin, Cunha, Sara I., Pietras, Kristian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5341292/
https://www.ncbi.nlm.nih.gov/pubmed/27741515
http://dx.doi.org/10.18632/oncotarget.12604
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author Eleftheriou, Nikolas M.
Sjölund, Jonas
Bocci, Matteo
Cortez, Eliane
Lee, Se-Jin
Cunha, Sara I.
Pietras, Kristian
author_facet Eleftheriou, Nikolas M.
Sjölund, Jonas
Bocci, Matteo
Cortez, Eliane
Lee, Se-Jin
Cunha, Sara I.
Pietras, Kristian
author_sort Eleftheriou, Nikolas M.
collection PubMed
description Angiogenesis occurs early in tumor development, sustains primary tumor growth and provides a route for metastatic escape. The TGF-β family receptors modulate angiogenesis via endothelial-cell specific pathways. Here we investigate the interaction of two such receptors, ALK1 and endoglin, in pancreatic neuroendocrine tumors (PanNET). Independently, ALK1 and endoglin deficiencies exhibited genetically divergent phenotypes, while both highly correlate to an endothelial metagene in human and mouse PanNETs. A concurrent deficiency of both receptors synergistically decreased tumor burden to a greater extent than either individual knockdown. Furthermore, the knockout of Gdf2 (BMP9), the primary ligand for ALK1 and endoglin, exhibited a mixed phenotype from each of ALK1 and endoglin deficiencies; overall primary tumor burden decreased, but hepatic metastases increased. Tumors lacking BMP9 display a hyperbranching vasculature, and an increase in vascular mesenchymal-marker expression, which may be implicit in the increase in metastases. Taken together, our work cautions against singular blockade of BMP9 and instead demonstrates the utility of dual blockade of ALK1 and endoglin as a strategy for anti-angiogenic therapy in PanNET.
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spelling pubmed-53412922017-03-08 Compound genetically engineered mouse models of cancer reveal dual targeting of ALK1 and endoglin as a synergistic opportunity to impinge on angiogenic TGF-β signaling Eleftheriou, Nikolas M. Sjölund, Jonas Bocci, Matteo Cortez, Eliane Lee, Se-Jin Cunha, Sara I. Pietras, Kristian Oncotarget Research Paper Angiogenesis occurs early in tumor development, sustains primary tumor growth and provides a route for metastatic escape. The TGF-β family receptors modulate angiogenesis via endothelial-cell specific pathways. Here we investigate the interaction of two such receptors, ALK1 and endoglin, in pancreatic neuroendocrine tumors (PanNET). Independently, ALK1 and endoglin deficiencies exhibited genetically divergent phenotypes, while both highly correlate to an endothelial metagene in human and mouse PanNETs. A concurrent deficiency of both receptors synergistically decreased tumor burden to a greater extent than either individual knockdown. Furthermore, the knockout of Gdf2 (BMP9), the primary ligand for ALK1 and endoglin, exhibited a mixed phenotype from each of ALK1 and endoglin deficiencies; overall primary tumor burden decreased, but hepatic metastases increased. Tumors lacking BMP9 display a hyperbranching vasculature, and an increase in vascular mesenchymal-marker expression, which may be implicit in the increase in metastases. Taken together, our work cautions against singular blockade of BMP9 and instead demonstrates the utility of dual blockade of ALK1 and endoglin as a strategy for anti-angiogenic therapy in PanNET. Impact Journals LLC 2016-10-12 /pmc/articles/PMC5341292/ /pubmed/27741515 http://dx.doi.org/10.18632/oncotarget.12604 Text en Copyright: © 2016 Eleftheriou et al. http://creativecommons.org/licenses/by/3.0/ 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 credited.
spellingShingle Research Paper
Eleftheriou, Nikolas M.
Sjölund, Jonas
Bocci, Matteo
Cortez, Eliane
Lee, Se-Jin
Cunha, Sara I.
Pietras, Kristian
Compound genetically engineered mouse models of cancer reveal dual targeting of ALK1 and endoglin as a synergistic opportunity to impinge on angiogenic TGF-β signaling
title Compound genetically engineered mouse models of cancer reveal dual targeting of ALK1 and endoglin as a synergistic opportunity to impinge on angiogenic TGF-β signaling
title_full Compound genetically engineered mouse models of cancer reveal dual targeting of ALK1 and endoglin as a synergistic opportunity to impinge on angiogenic TGF-β signaling
title_fullStr Compound genetically engineered mouse models of cancer reveal dual targeting of ALK1 and endoglin as a synergistic opportunity to impinge on angiogenic TGF-β signaling
title_full_unstemmed Compound genetically engineered mouse models of cancer reveal dual targeting of ALK1 and endoglin as a synergistic opportunity to impinge on angiogenic TGF-β signaling
title_short Compound genetically engineered mouse models of cancer reveal dual targeting of ALK1 and endoglin as a synergistic opportunity to impinge on angiogenic TGF-β signaling
title_sort compound genetically engineered mouse models of cancer reveal dual targeting of alk1 and endoglin as a synergistic opportunity to impinge on angiogenic tgf-β signaling
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5341292/
https://www.ncbi.nlm.nih.gov/pubmed/27741515
http://dx.doi.org/10.18632/oncotarget.12604
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