MYCN and HDAC5 transcriptionally repress CD9 to trigger invasion and metastasis in neuroblastoma

The systemic and resistant nature of metastatic neuroblastoma renders it largely incurable with current multimodal treatment. Clinical progression stems mainly from the increasing burden of metastatic colonization. Therapeutically inhibiting the migration-invasion-metastasis cascade would be of grea...

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Autores principales: Fabian, Johannes, Opitz, Desirée, Althoff, Kristina, Lodrini, Marco, Hero, Barbara, Volland, Ruth, Beckers, Anneleen, de Preter, Katleen, Decock, Anneleen, Patil, Nitin, Abba, Mohammed, Kopp-Schneider, Annette, Astrahantseff, Kathy, Wünschel, Jasmin, Pfeil, Sebastian, Ercu, Maria, Künkele, Annette, Hu, Jamie, Thole, Theresa, Schweizer, Leonille, Mechtersheimer, Gunhild, Carter, Daniel, Cheung, Belamy B., Popanda, Odilia, von Deimling, Andreas, Koster, Jan, Versteeg, Rogier, Schwab, Manfred, Marshall, Glenn M., Speleman, Frank, Erb, Ulrike, Zoeller, Margot, Allgayer, Heike, Simon, Thorsten, Fischer, Matthias, Kulozik, Andreas E., Eggert, Angelika, Witt, Olaf, Schulte, Johannes H., Deubzer, Hedwig E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Priority Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5341807/
https://www.ncbi.nlm.nih.gov/pubmed/27572323
http://dx.doi.org/10.18632/oncotarget.11662
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author Fabian, Johannes
Opitz, Desirée
Althoff, Kristina
Lodrini, Marco
Hero, Barbara
Volland, Ruth
Beckers, Anneleen
de Preter, Katleen
Decock, Anneleen
Patil, Nitin
Abba, Mohammed
Kopp-Schneider, Annette
Astrahantseff, Kathy
Wünschel, Jasmin
Pfeil, Sebastian
Ercu, Maria
Künkele, Annette
Hu, Jamie
Thole, Theresa
Schweizer, Leonille
Mechtersheimer, Gunhild
Carter, Daniel
Cheung, Belamy B.
Popanda, Odilia
von Deimling, Andreas
Koster, Jan
Versteeg, Rogier
Schwab, Manfred
Marshall, Glenn M.
Speleman, Frank
Erb, Ulrike
Zoeller, Margot
Allgayer, Heike
Simon, Thorsten
Fischer, Matthias
Kulozik, Andreas E.
Eggert, Angelika
Witt, Olaf
Schulte, Johannes H.
Deubzer, Hedwig E.
author_facet Fabian, Johannes
Opitz, Desirée
Althoff, Kristina
Lodrini, Marco
Hero, Barbara
Volland, Ruth
Beckers, Anneleen
de Preter, Katleen
Decock, Anneleen
Patil, Nitin
Abba, Mohammed
Kopp-Schneider, Annette
Astrahantseff, Kathy
Wünschel, Jasmin
Pfeil, Sebastian
Ercu, Maria
Künkele, Annette
Hu, Jamie
Thole, Theresa
Schweizer, Leonille
Mechtersheimer, Gunhild
Carter, Daniel
Cheung, Belamy B.
Popanda, Odilia
von Deimling, Andreas
Koster, Jan
Versteeg, Rogier
Schwab, Manfred
Marshall, Glenn M.
Speleman, Frank
Erb, Ulrike
Zoeller, Margot
Allgayer, Heike
Simon, Thorsten
Fischer, Matthias
Kulozik, Andreas E.
Eggert, Angelika
Witt, Olaf
Schulte, Johannes H.
Deubzer, Hedwig E.
author_sort Fabian, Johannes
collection PubMed
description The systemic and resistant nature of metastatic neuroblastoma renders it largely incurable with current multimodal treatment. Clinical progression stems mainly from the increasing burden of metastatic colonization. Therapeutically inhibiting the migration-invasion-metastasis cascade would be of great benefit, but the mechanisms driving this cycle are as yet poorly understood. In-depth transcriptome analyses and ChIP-qPCR identified the cell surface glycoprotein, CD9, as a major downstream player and direct target of the recently described GRHL1 tumor suppressor. CD9 is known to block or facilitate cancer cell motility and metastasis dependent upon entity. High-level CD9 expression in primary neuroblastomas correlated with patient survival and established markers for favorable disease. Low-level CD9 expression was an independent risk factor for adverse outcome. MYCN and HDAC5 colocalized to the CD9 promoter and repressed transcription. CD9 expression diminished with progressive tumor development in the TH-MYCN transgenic mouse model for neuroblastoma, and CD9 expression in neuroblastic tumors was far below that in ganglia from wildtype mice. Primary neuroblastomas lacking MYCN amplifications displayed differential CD9 promoter methylation in methyl-CpG-binding domain sequencing analyses, and high-level methylation was associated with advanced stage disease, supporting epigenetic regulation. Inducing CD9 expression in a SH-EP cell model inhibited migration and invasion in Boyden chamber assays. Enforced CD9 expression in neuroblastoma cells transplanted onto chicken chorioallantoic membranes strongly reduced metastasis to embryonic bone marrow. Combined treatment of neuroblastoma cells with HDAC/DNA methyltransferase inhibitors synergistically induced CD9 expression despite hypoxic, metabolic or cytotoxic stress. Our results show CD9 is a critical and indirectly druggable suppressor of the invasion-metastasis cycle in neuroblastoma.
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spelling pubmed-53418072017-03-23 MYCN and HDAC5 transcriptionally repress CD9 to trigger invasion and metastasis in neuroblastoma Fabian, Johannes Opitz, Desirée Althoff, Kristina Lodrini, Marco Hero, Barbara Volland, Ruth Beckers, Anneleen de Preter, Katleen Decock, Anneleen Patil, Nitin Abba, Mohammed Kopp-Schneider, Annette Astrahantseff, Kathy Wünschel, Jasmin Pfeil, Sebastian Ercu, Maria Künkele, Annette Hu, Jamie Thole, Theresa Schweizer, Leonille Mechtersheimer, Gunhild Carter, Daniel Cheung, Belamy B. Popanda, Odilia von Deimling, Andreas Koster, Jan Versteeg, Rogier Schwab, Manfred Marshall, Glenn M. Speleman, Frank Erb, Ulrike Zoeller, Margot Allgayer, Heike Simon, Thorsten Fischer, Matthias Kulozik, Andreas E. Eggert, Angelika Witt, Olaf Schulte, Johannes H. Deubzer, Hedwig E. Oncotarget Priority Research Paper The systemic and resistant nature of metastatic neuroblastoma renders it largely incurable with current multimodal treatment. Clinical progression stems mainly from the increasing burden of metastatic colonization. Therapeutically inhibiting the migration-invasion-metastasis cascade would be of great benefit, but the mechanisms driving this cycle are as yet poorly understood. In-depth transcriptome analyses and ChIP-qPCR identified the cell surface glycoprotein, CD9, as a major downstream player and direct target of the recently described GRHL1 tumor suppressor. CD9 is known to block or facilitate cancer cell motility and metastasis dependent upon entity. High-level CD9 expression in primary neuroblastomas correlated with patient survival and established markers for favorable disease. Low-level CD9 expression was an independent risk factor for adverse outcome. MYCN and HDAC5 colocalized to the CD9 promoter and repressed transcription. CD9 expression diminished with progressive tumor development in the TH-MYCN transgenic mouse model for neuroblastoma, and CD9 expression in neuroblastic tumors was far below that in ganglia from wildtype mice. Primary neuroblastomas lacking MYCN amplifications displayed differential CD9 promoter methylation in methyl-CpG-binding domain sequencing analyses, and high-level methylation was associated with advanced stage disease, supporting epigenetic regulation. Inducing CD9 expression in a SH-EP cell model inhibited migration and invasion in Boyden chamber assays. Enforced CD9 expression in neuroblastoma cells transplanted onto chicken chorioallantoic membranes strongly reduced metastasis to embryonic bone marrow. Combined treatment of neuroblastoma cells with HDAC/DNA methyltransferase inhibitors synergistically induced CD9 expression despite hypoxic, metabolic or cytotoxic stress. Our results show CD9 is a critical and indirectly druggable suppressor of the invasion-metastasis cycle in neuroblastoma. Impact Journals LLC 2016-08-27 /pmc/articles/PMC5341807/ /pubmed/27572323 http://dx.doi.org/10.18632/oncotarget.11662 Text en Copyright: © 2016 Fabian 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 Priority Research Paper
Fabian, Johannes
Opitz, Desirée
Althoff, Kristina
Lodrini, Marco
Hero, Barbara
Volland, Ruth
Beckers, Anneleen
de Preter, Katleen
Decock, Anneleen
Patil, Nitin
Abba, Mohammed
Kopp-Schneider, Annette
Astrahantseff, Kathy
Wünschel, Jasmin
Pfeil, Sebastian
Ercu, Maria
Künkele, Annette
Hu, Jamie
Thole, Theresa
Schweizer, Leonille
Mechtersheimer, Gunhild
Carter, Daniel
Cheung, Belamy B.
Popanda, Odilia
von Deimling, Andreas
Koster, Jan
Versteeg, Rogier
Schwab, Manfred
Marshall, Glenn M.
Speleman, Frank
Erb, Ulrike
Zoeller, Margot
Allgayer, Heike
Simon, Thorsten
Fischer, Matthias
Kulozik, Andreas E.
Eggert, Angelika
Witt, Olaf
Schulte, Johannes H.
Deubzer, Hedwig E.
MYCN and HDAC5 transcriptionally repress CD9 to trigger invasion and metastasis in neuroblastoma
title MYCN and HDAC5 transcriptionally repress CD9 to trigger invasion and metastasis in neuroblastoma
title_full MYCN and HDAC5 transcriptionally repress CD9 to trigger invasion and metastasis in neuroblastoma
title_fullStr MYCN and HDAC5 transcriptionally repress CD9 to trigger invasion and metastasis in neuroblastoma
title_full_unstemmed MYCN and HDAC5 transcriptionally repress CD9 to trigger invasion and metastasis in neuroblastoma
title_short MYCN and HDAC5 transcriptionally repress CD9 to trigger invasion and metastasis in neuroblastoma
title_sort mycn and hdac5 transcriptionally repress cd9 to trigger invasion and metastasis in neuroblastoma
topic Priority Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5341807/
https://www.ncbi.nlm.nih.gov/pubmed/27572323
http://dx.doi.org/10.18632/oncotarget.11662
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