MYCN amplification drives an aggressive form of spinal ependymoma

Spinal ependymal tumors form a histologically and molecularly heterogeneous group of tumors with generally good prognosis. However, their treatment can be challenging if infiltration of the spinal cord or dissemination throughout the central nervous system (CNS) occurs and, in these cases, clinical...

Descripción completa

Detalles Bibliográficos
Autores principales: Ghasemi, David R., Sill, Martin, Okonechnikov, Konstantin, Korshunov, Andrey, Yip, Stephen, Schutz, Peter W., Scheie, David, Kruse, Anders, Harter, Patrick N., Kastelan, Marina, Wagner, Marlies, Hartmann, Christian, Benzel, Julia, Maass, Kendra K., Khasraw, Mustafa, Sträter, Ronald, Thomas, Christian, Paulus, Werner, Kratz, Christian P., Witt, Hendrik, Kawauchi, Daisuke, Herold-Mende, Christel, Sahm, Felix, Brandner, Sebastian, Kool, Marcel, Jones, David T. W., von Deimling, Andreas, Pfister, Stefan M., Reuss, David E., Pajtler, Kristian W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Berlin Heidelberg 2019
Materias:
Original Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6851394/
https://www.ncbi.nlm.nih.gov/pubmed/31414211
http://dx.doi.org/10.1007/s00401-019-02056-2
_version_ 1783469626555891712
author Ghasemi, David R.
Sill, Martin
Okonechnikov, Konstantin
Korshunov, Andrey
Yip, Stephen
Schutz, Peter W.
Scheie, David
Kruse, Anders
Harter, Patrick N.
Kastelan, Marina
Wagner, Marlies
Hartmann, Christian
Benzel, Julia
Maass, Kendra K.
Khasraw, Mustafa
Sträter, Ronald
Thomas, Christian
Paulus, Werner
Kratz, Christian P.
Witt, Hendrik
Kawauchi, Daisuke
Herold-Mende, Christel
Sahm, Felix
Brandner, Sebastian
Kool, Marcel
Jones, David T. W.
von Deimling, Andreas
Pfister, Stefan M.
Reuss, David E.
Pajtler, Kristian W.
author_facet Ghasemi, David R.
Sill, Martin
Okonechnikov, Konstantin
Korshunov, Andrey
Yip, Stephen
Schutz, Peter W.
Scheie, David
Kruse, Anders
Harter, Patrick N.
Kastelan, Marina
Wagner, Marlies
Hartmann, Christian
Benzel, Julia
Maass, Kendra K.
Khasraw, Mustafa
Sträter, Ronald
Thomas, Christian
Paulus, Werner
Kratz, Christian P.
Witt, Hendrik
Kawauchi, Daisuke
Herold-Mende, Christel
Sahm, Felix
Brandner, Sebastian
Kool, Marcel
Jones, David T. W.
von Deimling, Andreas
Pfister, Stefan M.
Reuss, David E.
Pajtler, Kristian W.
author_sort Ghasemi, David R.
collection PubMed
description Spinal ependymal tumors form a histologically and molecularly heterogeneous group of tumors with generally good prognosis. However, their treatment can be challenging if infiltration of the spinal cord or dissemination throughout the central nervous system (CNS) occurs and, in these cases, clinical outcome remains poor. Here, we describe a new and relatively rare subgroup of spinal ependymal tumors identified using DNA methylation profiling that is distinct from other molecular subgroups of ependymoma. Copy number variation plots derived from DNA methylation arrays showed MYCN amplification as a characteristic genetic alteration in all cases of our cohort (n = 13), which was subsequently validated using fluorescence in situ hybridization. The histological diagnosis was anaplastic ependymoma (WHO Grade III) in ten cases and classic ependymoma (WHO Grade II) in three cases. Histological re-evaluation in five primary tumors and seven relapses showed characteristic histological features of ependymoma, namely pseudorosettes, GFAP- and EMA positivity. Electron microscopy revealed cilia, complex intercellular junctions and intermediate filaments in a representative sample. Taking these findings into account, we suggest to designate this molecular subgroup spinal ependymoma with MYCN amplification, SP-EPN-MYCN. SP-EPN-MYCN tumors showed distinct growth patterns with intradural, extramedullary localization mostly within the thoracic and cervical spine, diffuse leptomeningeal spread throughout the whole CNS and infiltrative invasion of the spinal cord. Dissemination was observed in 100% of cases. Despite high-intensity treatment, SP-EPN-MYCN showed significantly worse median progression free survival (PFS) (17 months) and median overall survival (OS) (87 months) than all other previously described molecular spinal ependymoma subgroups. OS and PFS were similar to supratentorial ependymoma with RELA-fusion (ST-EPN-RELA) and posterior fossa ependymoma A (PF-EPN-A), further highlighting the aggressiveness of this distinct new subgroup. We, therefore, propose to establish SP-EPN-MYCN as a new molecular subgroup in ependymoma and advocate for testing newly diagnosed spinal ependymal tumors for MYCN amplification. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s00401-019-02056-2) contains supplementary material, which is available to authorized users.
format Online
Article
Text
id pubmed-6851394
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Springer Berlin Heidelberg
record_format MEDLINE/PubMed
spelling pubmed-68513942019-12-03 MYCN amplification drives an aggressive form of spinal ependymoma Ghasemi, David R. Sill, Martin Okonechnikov, Konstantin Korshunov, Andrey Yip, Stephen Schutz, Peter W. Scheie, David Kruse, Anders Harter, Patrick N. Kastelan, Marina Wagner, Marlies Hartmann, Christian Benzel, Julia Maass, Kendra K. Khasraw, Mustafa Sträter, Ronald Thomas, Christian Paulus, Werner Kratz, Christian P. Witt, Hendrik Kawauchi, Daisuke Herold-Mende, Christel Sahm, Felix Brandner, Sebastian Kool, Marcel Jones, David T. W. von Deimling, Andreas Pfister, Stefan M. Reuss, David E. Pajtler, Kristian W. Acta Neuropathol Original Paper Spinal ependymal tumors form a histologically and molecularly heterogeneous group of tumors with generally good prognosis. However, their treatment can be challenging if infiltration of the spinal cord or dissemination throughout the central nervous system (CNS) occurs and, in these cases, clinical outcome remains poor. Here, we describe a new and relatively rare subgroup of spinal ependymal tumors identified using DNA methylation profiling that is distinct from other molecular subgroups of ependymoma. Copy number variation plots derived from DNA methylation arrays showed MYCN amplification as a characteristic genetic alteration in all cases of our cohort (n = 13), which was subsequently validated using fluorescence in situ hybridization. The histological diagnosis was anaplastic ependymoma (WHO Grade III) in ten cases and classic ependymoma (WHO Grade II) in three cases. Histological re-evaluation in five primary tumors and seven relapses showed characteristic histological features of ependymoma, namely pseudorosettes, GFAP- and EMA positivity. Electron microscopy revealed cilia, complex intercellular junctions and intermediate filaments in a representative sample. Taking these findings into account, we suggest to designate this molecular subgroup spinal ependymoma with MYCN amplification, SP-EPN-MYCN. SP-EPN-MYCN tumors showed distinct growth patterns with intradural, extramedullary localization mostly within the thoracic and cervical spine, diffuse leptomeningeal spread throughout the whole CNS and infiltrative invasion of the spinal cord. Dissemination was observed in 100% of cases. Despite high-intensity treatment, SP-EPN-MYCN showed significantly worse median progression free survival (PFS) (17 months) and median overall survival (OS) (87 months) than all other previously described molecular spinal ependymoma subgroups. OS and PFS were similar to supratentorial ependymoma with RELA-fusion (ST-EPN-RELA) and posterior fossa ependymoma A (PF-EPN-A), further highlighting the aggressiveness of this distinct new subgroup. We, therefore, propose to establish SP-EPN-MYCN as a new molecular subgroup in ependymoma and advocate for testing newly diagnosed spinal ependymal tumors for MYCN amplification. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s00401-019-02056-2) contains supplementary material, which is available to authorized users. Springer Berlin Heidelberg 2019-08-14 2019 /pmc/articles/PMC6851394/ /pubmed/31414211 http://dx.doi.org/10.1007/s00401-019-02056-2 Text en © The Author(s) 2019 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.
spellingShingle Original Paper
Ghasemi, David R.
Sill, Martin
Okonechnikov, Konstantin
Korshunov, Andrey
Yip, Stephen
Schutz, Peter W.
Scheie, David
Kruse, Anders
Harter, Patrick N.
Kastelan, Marina
Wagner, Marlies
Hartmann, Christian
Benzel, Julia
Maass, Kendra K.
Khasraw, Mustafa
Sträter, Ronald
Thomas, Christian
Paulus, Werner
Kratz, Christian P.
Witt, Hendrik
Kawauchi, Daisuke
Herold-Mende, Christel
Sahm, Felix
Brandner, Sebastian
Kool, Marcel
Jones, David T. W.
von Deimling, Andreas
Pfister, Stefan M.
Reuss, David E.
Pajtler, Kristian W.
MYCN amplification drives an aggressive form of spinal ependymoma
title MYCN amplification drives an aggressive form of spinal ependymoma
title_full MYCN amplification drives an aggressive form of spinal ependymoma
title_fullStr MYCN amplification drives an aggressive form of spinal ependymoma
title_full_unstemmed MYCN amplification drives an aggressive form of spinal ependymoma
title_short MYCN amplification drives an aggressive form of spinal ependymoma
title_sort mycn amplification drives an aggressive form of spinal ependymoma
topic Original Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6851394/
https://www.ncbi.nlm.nih.gov/pubmed/31414211
http://dx.doi.org/10.1007/s00401-019-02056-2
work_keys_str_mv AT ghasemidavidr mycnamplificationdrivesanaggressiveformofspinalependymoma
AT sillmartin mycnamplificationdrivesanaggressiveformofspinalependymoma
AT okonechnikovkonstantin mycnamplificationdrivesanaggressiveformofspinalependymoma
AT korshunovandrey mycnamplificationdrivesanaggressiveformofspinalependymoma
AT yipstephen mycnamplificationdrivesanaggressiveformofspinalependymoma
AT schutzpeterw mycnamplificationdrivesanaggressiveformofspinalependymoma
AT scheiedavid mycnamplificationdrivesanaggressiveformofspinalependymoma
AT kruseanders mycnamplificationdrivesanaggressiveformofspinalependymoma
AT harterpatrickn mycnamplificationdrivesanaggressiveformofspinalependymoma
AT kastelanmarina mycnamplificationdrivesanaggressiveformofspinalependymoma
AT wagnermarlies mycnamplificationdrivesanaggressiveformofspinalependymoma
AT hartmannchristian mycnamplificationdrivesanaggressiveformofspinalependymoma
AT benzeljulia mycnamplificationdrivesanaggressiveformofspinalependymoma
AT maasskendrak mycnamplificationdrivesanaggressiveformofspinalependymoma
AT khasrawmustafa mycnamplificationdrivesanaggressiveformofspinalependymoma
AT straterronald mycnamplificationdrivesanaggressiveformofspinalependymoma
AT thomaschristian mycnamplificationdrivesanaggressiveformofspinalependymoma
AT pauluswerner mycnamplificationdrivesanaggressiveformofspinalependymoma
AT kratzchristianp mycnamplificationdrivesanaggressiveformofspinalependymoma
AT witthendrik mycnamplificationdrivesanaggressiveformofspinalependymoma
AT kawauchidaisuke mycnamplificationdrivesanaggressiveformofspinalependymoma
AT heroldmendechristel mycnamplificationdrivesanaggressiveformofspinalependymoma
AT sahmfelix mycnamplificationdrivesanaggressiveformofspinalependymoma
AT brandnersebastian mycnamplificationdrivesanaggressiveformofspinalependymoma
AT koolmarcel mycnamplificationdrivesanaggressiveformofspinalependymoma
AT jonesdavidtw mycnamplificationdrivesanaggressiveformofspinalependymoma
AT vondeimlingandreas mycnamplificationdrivesanaggressiveformofspinalependymoma
AT pfisterstefanm mycnamplificationdrivesanaggressiveformofspinalependymoma
AT reussdavide mycnamplificationdrivesanaggressiveformofspinalependymoma
AT pajtlerkristianw mycnamplificationdrivesanaggressiveformofspinalependymoma

Ejemplares similares