Loss of Trop2 causes ErbB3 activation through a neuregulin-1-dependent mechanism in the mesenchymal subtype of HNSCC

In head and neck squamous cell cancer (HNSCC), four intrinsic subtypes (or groups) have been identified, and each one possesses a unique biology that will require specific treatment strategies. We previously reported that mesenchymal (group 2) tumors exhibit reduced levels of Trop2 expression. In th...

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Autores principales: Zhang, Kaihua, Jones, Lamont, Lim, Sora, Maher, Christopher A., Adkins, Douglas, Lewis, James, Kimple, Randall J., Fertig, Elana J., Chung, Christine H., Herrlich, Andreas, Ellis, Matthew J., Van Tine, Brian A., Michel, Loren S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2014
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4253434/
https://www.ncbi.nlm.nih.gov/pubmed/25238142
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author Zhang, Kaihua
Jones, Lamont
Lim, Sora
Maher, Christopher A.
Adkins, Douglas
Lewis, James
Kimple, Randall J.
Fertig, Elana J.
Chung, Christine H.
Herrlich, Andreas
Ellis, Matthew J.
Van Tine, Brian A.
Michel, Loren S.
author_facet Zhang, Kaihua
Jones, Lamont
Lim, Sora
Maher, Christopher A.
Adkins, Douglas
Lewis, James
Kimple, Randall J.
Fertig, Elana J.
Chung, Christine H.
Herrlich, Andreas
Ellis, Matthew J.
Van Tine, Brian A.
Michel, Loren S.
author_sort Zhang, Kaihua
collection PubMed
description In head and neck squamous cell cancer (HNSCC), four intrinsic subtypes (or groups) have been identified, and each one possesses a unique biology that will require specific treatment strategies. We previously reported that mesenchymal (group 2) tumors exhibit reduced levels of Trop2 expression. In this study, we investigated the functional role of Trop2 in HNSCC and find that loss results in autocrine activation of the EGFR family member ErbB3 via neuregulin-1. Trop2 localizes to both the cell surface and cytosol of HNSCC cells and forms a complex with neuregulin-1, which is predominantly cytosolic. Inactivation of Trop2 increases the concentration of neuregulin-1 at the cell surface where it is cleaved to activate ErbB3. In primary HNSCC, detection of ErbB3 activation was limited to Trop2 negative tumors. An analysis of the Cancer Genome Atlas (TCGA) HNSCC dataset confirms enrichment for ErbB3 activity in mesenchymal tumors. Notably, Trop2 loss triggers sensitivity to anti-ErbB3 antibodies, which results in reduced proliferation and tumorigenic growth of Trop2 negative HNSCC cancer cells. These results uncover a molecular mechanism by which tumor cells control the amount of cell-surface neuregulin-1 available for cleavage and ErbB3 activation. Moreover, we demonstrate that Trop2 is a potential surrogate biomarker to identify tumors with ErbB3 activation and may therefore respond to anti-ErbB3 therapeutics.
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spelling pubmed-42534342014-12-03 Loss of Trop2 causes ErbB3 activation through a neuregulin-1-dependent mechanism in the mesenchymal subtype of HNSCC Zhang, Kaihua Jones, Lamont Lim, Sora Maher, Christopher A. Adkins, Douglas Lewis, James Kimple, Randall J. Fertig, Elana J. Chung, Christine H. Herrlich, Andreas Ellis, Matthew J. Van Tine, Brian A. Michel, Loren S. Oncotarget Research Paper In head and neck squamous cell cancer (HNSCC), four intrinsic subtypes (or groups) have been identified, and each one possesses a unique biology that will require specific treatment strategies. We previously reported that mesenchymal (group 2) tumors exhibit reduced levels of Trop2 expression. In this study, we investigated the functional role of Trop2 in HNSCC and find that loss results in autocrine activation of the EGFR family member ErbB3 via neuregulin-1. Trop2 localizes to both the cell surface and cytosol of HNSCC cells and forms a complex with neuregulin-1, which is predominantly cytosolic. Inactivation of Trop2 increases the concentration of neuregulin-1 at the cell surface where it is cleaved to activate ErbB3. In primary HNSCC, detection of ErbB3 activation was limited to Trop2 negative tumors. An analysis of the Cancer Genome Atlas (TCGA) HNSCC dataset confirms enrichment for ErbB3 activity in mesenchymal tumors. Notably, Trop2 loss triggers sensitivity to anti-ErbB3 antibodies, which results in reduced proliferation and tumorigenic growth of Trop2 negative HNSCC cancer cells. These results uncover a molecular mechanism by which tumor cells control the amount of cell-surface neuregulin-1 available for cleavage and ErbB3 activation. Moreover, we demonstrate that Trop2 is a potential surrogate biomarker to identify tumors with ErbB3 activation and may therefore respond to anti-ErbB3 therapeutics. Impact Journals LLC 2014-09-02 /pmc/articles/PMC4253434/ /pubmed/25238142 Text en Copyright: © 2014 Zhang et al. http://creativecommons.org/licenses/by/2.5/ 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
Zhang, Kaihua
Jones, Lamont
Lim, Sora
Maher, Christopher A.
Adkins, Douglas
Lewis, James
Kimple, Randall J.
Fertig, Elana J.
Chung, Christine H.
Herrlich, Andreas
Ellis, Matthew J.
Van Tine, Brian A.
Michel, Loren S.
Loss of Trop2 causes ErbB3 activation through a neuregulin-1-dependent mechanism in the mesenchymal subtype of HNSCC
title Loss of Trop2 causes ErbB3 activation through a neuregulin-1-dependent mechanism in the mesenchymal subtype of HNSCC
title_full Loss of Trop2 causes ErbB3 activation through a neuregulin-1-dependent mechanism in the mesenchymal subtype of HNSCC
title_fullStr Loss of Trop2 causes ErbB3 activation through a neuregulin-1-dependent mechanism in the mesenchymal subtype of HNSCC
title_full_unstemmed Loss of Trop2 causes ErbB3 activation through a neuregulin-1-dependent mechanism in the mesenchymal subtype of HNSCC
title_short Loss of Trop2 causes ErbB3 activation through a neuregulin-1-dependent mechanism in the mesenchymal subtype of HNSCC
title_sort loss of trop2 causes erbb3 activation through a neuregulin-1-dependent mechanism in the mesenchymal subtype of hnscc
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4253434/
https://www.ncbi.nlm.nih.gov/pubmed/25238142
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