Medulloblastoma subgroups remain stable across primary and metastatic compartments

Xin Wang; Adrian M. Dubuc; Vijay Ramaswamy; Stephen Mack; Deena M. A. Gendoo; Marc Remke; Xiaochong Wu; Livia Garzia; Betty Luu; Florence Cavalli; John Peacock; Borja López; Patryk Skowron; David Zagzag; David Lyden; Caitlin Hoffman; Yoon-Jae Cho; Charles Eberhart; Tobey MacDonald; Xiao-Nan Li; Timothy Van Meter; Paul A. Northcott; Benjamin Haibe-Kains; Cynthia Hawkins; James T. Rutka; Eric Bouffet; Stefan M. Pfister; Andrey Korshunov; Michael D. Taylor

doi:10.1007/s00401-015-1389-0

Medulloblastoma subgroups remain stable across primary and metastatic compartments

Xin Wang, Adrian M. Dubuc, Vijay Ramaswamy, Stephen Mack, Deena M. A. Gendoo, Marc Remke, Xiaochong Wu, Livia Garzia, Betty Luu, Florence Cavalli, John Peacock, Borja López, Patryk Skowron, David Zagzag, David Lyden, Caitlin Hoffman, Yoon-Jae Cho, Charles Eberhart, Tobey MacDonald, Xiao-Nan LiTimothy Van Meter, Paul A. Northcott, Benjamin Haibe-Kains, Cynthia Hawkins, James T. Rutka, Eric Bouffet, Stefan M. Pfister, Andrey Korshunov, Michael D. Taylor

Cancer and Genomic Sciences

Research output: Contribution to journal › Article › peer-review

53 Citations (Scopus)

Abstract

Medulloblastoma comprises four distinct molecular variants with distinct genetics, transcriptomes, and outcomes. Subgroup affiliation has been previously shown to remain stable at the time of recurrence, which likely reflects their distinct cells of origin. However, a therapeutically relevant question that remains unanswered is subgroup stability in the metastatic compartment. We assembled a cohort of 12-paired primary-metastatic tumors collected in the MAGIC consortium, and established their molecular subgroup affiliation by performing integrative gene expression and DNA methylation analysis. Frozen tissues were collected and profiled using Affymetrix gene expression arrays and Illumina methylation arrays. Class prediction and hierarchical clustering were performed using existing published datasets. Our molecular analysis, using consensus integrative genomic data, establishes the unequivocal maintenance of molecular subgroup affiliation in metastatic medulloblastoma. We further validated these findings by interrogating a non-overlapping cohort of 19 pairs of primary-metastatic tumors from the Burdenko Neurosurgical Institute using an orthogonal technique of immunohistochemical staining. This investigation represents the largest reported primary-metastatic paired cohort profiled to date and provides a unique opportunity to evaluate subgroup-specific molecular aberrations within the metastatic compartment. Our findings further support the hypothesis that medulloblastoma subgroups arise from distinct cells of origin, which are carried forward from ontogeny to oncology.

Original language	English
Pages (from-to)	449-457
Number of pages	9
Journal	Acta Neuropathologica
Volume	129
Issue number	3
Early online date	21 Jan 2015
DOIs	https://doi.org/10.1007/s00401-015-1389-0
Publication status	Published - Mar 2015

Keywords

Medulloblastoma
Metastasis
Molecular subgroups
Integrative genomics
Gene expression
DNA methylation

Access to Document

10.1007/s00401-015-1389-0Licence: None: All rights reserved

https://doi.org/10.1007/s00401-015-1389-0Licence: None: All rights reserved

Cite this

Wang, X., Dubuc, A. M., Ramaswamy, V., Mack, S., Gendoo, D. M. A., Remke, M., Wu, X., Garzia, L., Luu, B., Cavalli, F., Peacock, J., López, B., Skowron, P., Zagzag, D., Lyden, D., Hoffman, C., Cho, Y.-J., Eberhart, C., MacDonald, T., ... Taylor, M. D. (2015). Medulloblastoma subgroups remain stable across primary and metastatic compartments. Acta Neuropathologica, 129(3), 449-457. https://doi.org/10.1007/s00401-015-1389-0

@article{66848c435f8c4f4abde3ce2ffa9e1da2,

title = "Medulloblastoma subgroups remain stable across primary and metastatic compartments",

abstract = "Medulloblastoma comprises four distinct molecular variants with distinct genetics, transcriptomes, and outcomes. Subgroup affiliation has been previously shown to remain stable at the time of recurrence, which likely reflects their distinct cells of origin. However, a therapeutically relevant question that remains unanswered is subgroup stability in the metastatic compartment. We assembled a cohort of 12-paired primary-metastatic tumors collected in the MAGIC consortium, and established their molecular subgroup affiliation by performing integrative gene expression and DNA methylation analysis. Frozen tissues were collected and profiled using Affymetrix gene expression arrays and Illumina methylation arrays. Class prediction and hierarchical clustering were performed using existing published datasets. Our molecular analysis, using consensus integrative genomic data, establishes the unequivocal maintenance of molecular subgroup affiliation in metastatic medulloblastoma. We further validated these findings by interrogating a non-overlapping cohort of 19 pairs of primary-metastatic tumors from the Burdenko Neurosurgical Institute using an orthogonal technique of immunohistochemical staining. This investigation represents the largest reported primary-metastatic paired cohort profiled to date and provides a unique opportunity to evaluate subgroup-specific molecular aberrations within the metastatic compartment. Our findings further support the hypothesis that medulloblastoma subgroups arise from distinct cells of origin, which are carried forward from ontogeny to oncology.",

keywords = "Medulloblastoma, Metastasis, Molecular subgroups, Integrative genomics, Gene expression, DNA methylation",

author = "Xin Wang and Dubuc, {Adrian M.} and Vijay Ramaswamy and Stephen Mack and Gendoo, {Deena M. A.} and Marc Remke and Xiaochong Wu and Livia Garzia and Betty Luu and Florence Cavalli and John Peacock and Borja L{\'o}pez and Patryk Skowron and David Zagzag and David Lyden and Caitlin Hoffman and Yoon-Jae Cho and Charles Eberhart and Tobey MacDonald and Xiao-Nan Li and {Van Meter}, Timothy and Northcott, {Paul A.} and Benjamin Haibe-Kains and Cynthia Hawkins and Rutka, {James T.} and Eric Bouffet and Pfister, {Stefan M.} and Andrey Korshunov and Taylor, {Michael D.}",

year = "2015",

month = mar,

doi = "10.1007/s00401-015-1389-0",

language = "English",

volume = "129",

pages = "449--457",

journal = "Acta Neuropathologica",

issn = "1432-0533",

publisher = "Springer",

number = "3",

}

Wang, X, Dubuc, AM, Ramaswamy, V, Mack, S, Gendoo, DMA, Remke, M, Wu, X, Garzia, L, Luu, B, Cavalli, F, Peacock, J, López, B, Skowron, P, Zagzag, D, Lyden, D, Hoffman, C, Cho, Y-J, Eberhart, C, MacDonald, T, Li, X-N, Van Meter, T, Northcott, PA, Haibe-Kains, B, Hawkins, C, Rutka, JT, Bouffet, E, Pfister, SM, Korshunov, A & Taylor, MD 2015, 'Medulloblastoma subgroups remain stable across primary and metastatic compartments', Acta Neuropathologica, vol. 129, no. 3, pp. 449-457. https://doi.org/10.1007/s00401-015-1389-0

TY - JOUR

T1 - Medulloblastoma subgroups remain stable across primary and metastatic compartments

AU - Wang, Xin

AU - Dubuc, Adrian M.

AU - Ramaswamy, Vijay

AU - Mack, Stephen

AU - Gendoo, Deena M. A.

AU - Remke, Marc

AU - Wu, Xiaochong

AU - Garzia, Livia

AU - Luu, Betty

AU - Cavalli, Florence

AU - Peacock, John

AU - López, Borja

AU - Skowron, Patryk

AU - Zagzag, David

AU - Lyden, David

AU - Hoffman, Caitlin

AU - Cho, Yoon-Jae

AU - Eberhart, Charles

AU - MacDonald, Tobey

AU - Li, Xiao-Nan

AU - Van Meter, Timothy

AU - Northcott, Paul A.

AU - Haibe-Kains, Benjamin

AU - Hawkins, Cynthia

AU - Rutka, James T.

AU - Bouffet, Eric

AU - Pfister, Stefan M.

AU - Korshunov, Andrey

AU - Taylor, Michael D.

PY - 2015/3

Y1 - 2015/3

N2 - Medulloblastoma comprises four distinct molecular variants with distinct genetics, transcriptomes, and outcomes. Subgroup affiliation has been previously shown to remain stable at the time of recurrence, which likely reflects their distinct cells of origin. However, a therapeutically relevant question that remains unanswered is subgroup stability in the metastatic compartment. We assembled a cohort of 12-paired primary-metastatic tumors collected in the MAGIC consortium, and established their molecular subgroup affiliation by performing integrative gene expression and DNA methylation analysis. Frozen tissues were collected and profiled using Affymetrix gene expression arrays and Illumina methylation arrays. Class prediction and hierarchical clustering were performed using existing published datasets. Our molecular analysis, using consensus integrative genomic data, establishes the unequivocal maintenance of molecular subgroup affiliation in metastatic medulloblastoma. We further validated these findings by interrogating a non-overlapping cohort of 19 pairs of primary-metastatic tumors from the Burdenko Neurosurgical Institute using an orthogonal technique of immunohistochemical staining. This investigation represents the largest reported primary-metastatic paired cohort profiled to date and provides a unique opportunity to evaluate subgroup-specific molecular aberrations within the metastatic compartment. Our findings further support the hypothesis that medulloblastoma subgroups arise from distinct cells of origin, which are carried forward from ontogeny to oncology.

AB - Medulloblastoma comprises four distinct molecular variants with distinct genetics, transcriptomes, and outcomes. Subgroup affiliation has been previously shown to remain stable at the time of recurrence, which likely reflects their distinct cells of origin. However, a therapeutically relevant question that remains unanswered is subgroup stability in the metastatic compartment. We assembled a cohort of 12-paired primary-metastatic tumors collected in the MAGIC consortium, and established their molecular subgroup affiliation by performing integrative gene expression and DNA methylation analysis. Frozen tissues were collected and profiled using Affymetrix gene expression arrays and Illumina methylation arrays. Class prediction and hierarchical clustering were performed using existing published datasets. Our molecular analysis, using consensus integrative genomic data, establishes the unequivocal maintenance of molecular subgroup affiliation in metastatic medulloblastoma. We further validated these findings by interrogating a non-overlapping cohort of 19 pairs of primary-metastatic tumors from the Burdenko Neurosurgical Institute using an orthogonal technique of immunohistochemical staining. This investigation represents the largest reported primary-metastatic paired cohort profiled to date and provides a unique opportunity to evaluate subgroup-specific molecular aberrations within the metastatic compartment. Our findings further support the hypothesis that medulloblastoma subgroups arise from distinct cells of origin, which are carried forward from ontogeny to oncology.

KW - Medulloblastoma

KW - Metastasis

KW - Molecular subgroups

KW - Integrative genomics

KW - Gene expression

KW - DNA methylation

U2 - 10.1007/s00401-015-1389-0

DO - 10.1007/s00401-015-1389-0

M3 - Article

SN - 1432-0533

VL - 129

SP - 449

EP - 457

JO - Acta Neuropathologica

JF - Acta Neuropathologica

IS - 3

ER -

Medulloblastoma subgroups remain stable across primary and metastatic compartments

Abstract

Keywords

Access to Document

Fingerprint

Cite this