MEDB-78. Unified rhombic lip origins of Group 3 and Group 4 medulloblastoma

Identification and characterization of lineage-specific beginnings of distinct medulloblastoma (MB) subgroups is a fundamental challenge in the field. Genetically engineered mouse models and cross-species transcriptomics have provided mounting evidence of discrete, subgroup-specific developmental or...

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Autores principales: Smith, Kyle, Bihannic, Laure, Gudenas, Brian, Gao, Qingsong, Haldipur, Parthiv, Tao, Ran, Iskusnykh, Igor, Chizhikov, Viktor, Scoggins, Matthew, Zhang, Silu, Edwards, Angela, Deng, Mei, Glass, Ian, Overman, Lynne, Millman, Jake, Sjoboen, Alexandria, Hadley, Jennifer, Mankad, Kshitij, Onar-Thomas, Arzu, Gajjar, Amar, Robinson, Giles, Aldinger, Kimberly, Hovestadt, Volker, Tillman, Heather, Orr, Brent, Patay, Zoltán, Millen, Kathleen, Northcott, Paul
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Medulloblastoma
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9165102/
http://dx.doi.org/10.1093/neuonc/noac079.452
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author Smith, Kyle
Bihannic, Laure
Gudenas, Brian
Gao, Qingsong
Haldipur, Parthiv
Tao, Ran
Iskusnykh, Igor
Chizhikov, Viktor
Scoggins, Matthew
Zhang, Silu
Edwards, Angela
Deng, Mei
Glass, Ian
Overman, Lynne
Millman, Jake
Sjoboen, Alexandria
Hadley, Jennifer
Mankad, Kshitij
Onar-Thomas, Arzu
Gajjar, Amar
Robinson, Giles
Aldinger, Kimberly
Hovestadt, Volker
Tillman, Heather
Orr, Brent
Patay, Zoltán
Millen, Kathleen
Northcott, Paul
author_facet Smith, Kyle
Bihannic, Laure
Gudenas, Brian
Gao, Qingsong
Haldipur, Parthiv
Tao, Ran
Iskusnykh, Igor
Chizhikov, Viktor
Scoggins, Matthew
Zhang, Silu
Edwards, Angela
Deng, Mei
Glass, Ian
Overman, Lynne
Millman, Jake
Sjoboen, Alexandria
Hadley, Jennifer
Mankad, Kshitij
Onar-Thomas, Arzu
Gajjar, Amar
Robinson, Giles
Aldinger, Kimberly
Hovestadt, Volker
Tillman, Heather
Orr, Brent
Patay, Zoltán
Millen, Kathleen
Northcott, Paul
author_sort Smith, Kyle
collection PubMed
description Identification and characterization of lineage-specific beginnings of distinct medulloblastoma (MB) subgroups is a fundamental challenge in the field. Genetically engineered mouse models and cross-species transcriptomics have provided mounting evidence of discrete, subgroup-specific developmental origins. Likewise, murine single-cell transcriptional atlases of cerebellar development have recently provided further clues into MB subgroup origins, particularly for poorly defined Group 3 and Group 4-MB. However, initial studies were underpowered to characterize rare populations and lacked robust validation, resulting in incomplete findings. Herein, we leveraged a large harmonized murine cerebellar atlas, targeted lineage enrichment, and integrative multi-omic strategies to deeply dissect MB origins. Isolation of spatially and temporally discrete developmental trajectories of key glutamatergic lineages born out of the murine upper rhombic lip provided an enhanced reference for mapping MB subgroup origins, especially for Group 3 and Group 4-MB. However, human-specific anatomic and cellular complexity, particularly within the rhombic lip germinal zone complicated murine-derived inferences. Further tumor-normal integrations using a novel single-cell atlas of the human fetal cerebellum, companioned with laser-capture micro-dissected transcriptional and epigenetic datasets, reinforced developmental insights extracted from candidate murine cerebellar lineages. Characterization of compartment-specific transcriptional signatures identified in the human upper rhombic lip implicated convergent cellular correlates of Group 3 and Group 4-MB, suggestive of a common developmental trajectory underlying their ancestry. Systematic imaging review and 3D summarization of a large clinical trial series of patient tumors, coupled with our advanced insights into developmental signatures, substantiated subgroup-specific tumor location patterns observed at diagnosis. Together, our results strongly implicate a common lineage trajectory of the upper rhombic lip as the probable origin of Group 3 and Group 4-MB. These important findings provide unprecedented opportunities to explore context-dependent mechanisms of MB pathogenesis and will foster generation of improved preclinical models that more faithfully recapitulate tumor biology.
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spelling pubmed-91651022022-06-05 MEDB-78. Unified rhombic lip origins of Group 3 and Group 4 medulloblastoma Smith, Kyle Bihannic, Laure Gudenas, Brian Gao, Qingsong Haldipur, Parthiv Tao, Ran Iskusnykh, Igor Chizhikov, Viktor Scoggins, Matthew Zhang, Silu Edwards, Angela Deng, Mei Glass, Ian Overman, Lynne Millman, Jake Sjoboen, Alexandria Hadley, Jennifer Mankad, Kshitij Onar-Thomas, Arzu Gajjar, Amar Robinson, Giles Aldinger, Kimberly Hovestadt, Volker Tillman, Heather Orr, Brent Patay, Zoltán Millen, Kathleen Northcott, Paul Neuro Oncol Medulloblastoma Identification and characterization of lineage-specific beginnings of distinct medulloblastoma (MB) subgroups is a fundamental challenge in the field. Genetically engineered mouse models and cross-species transcriptomics have provided mounting evidence of discrete, subgroup-specific developmental origins. Likewise, murine single-cell transcriptional atlases of cerebellar development have recently provided further clues into MB subgroup origins, particularly for poorly defined Group 3 and Group 4-MB. However, initial studies were underpowered to characterize rare populations and lacked robust validation, resulting in incomplete findings. Herein, we leveraged a large harmonized murine cerebellar atlas, targeted lineage enrichment, and integrative multi-omic strategies to deeply dissect MB origins. Isolation of spatially and temporally discrete developmental trajectories of key glutamatergic lineages born out of the murine upper rhombic lip provided an enhanced reference for mapping MB subgroup origins, especially for Group 3 and Group 4-MB. However, human-specific anatomic and cellular complexity, particularly within the rhombic lip germinal zone complicated murine-derived inferences. Further tumor-normal integrations using a novel single-cell atlas of the human fetal cerebellum, companioned with laser-capture micro-dissected transcriptional and epigenetic datasets, reinforced developmental insights extracted from candidate murine cerebellar lineages. Characterization of compartment-specific transcriptional signatures identified in the human upper rhombic lip implicated convergent cellular correlates of Group 3 and Group 4-MB, suggestive of a common developmental trajectory underlying their ancestry. Systematic imaging review and 3D summarization of a large clinical trial series of patient tumors, coupled with our advanced insights into developmental signatures, substantiated subgroup-specific tumor location patterns observed at diagnosis. Together, our results strongly implicate a common lineage trajectory of the upper rhombic lip as the probable origin of Group 3 and Group 4-MB. These important findings provide unprecedented opportunities to explore context-dependent mechanisms of MB pathogenesis and will foster generation of improved preclinical models that more faithfully recapitulate tumor biology. Oxford University Press 2022-06-03 /pmc/articles/PMC9165102/ http://dx.doi.org/10.1093/neuonc/noac079.452 Text en © The Author(s) 2022. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Medulloblastoma
Smith, Kyle
Bihannic, Laure
Gudenas, Brian
Gao, Qingsong
Haldipur, Parthiv
Tao, Ran
Iskusnykh, Igor
Chizhikov, Viktor
Scoggins, Matthew
Zhang, Silu
Edwards, Angela
Deng, Mei
Glass, Ian
Overman, Lynne
Millman, Jake
Sjoboen, Alexandria
Hadley, Jennifer
Mankad, Kshitij
Onar-Thomas, Arzu
Gajjar, Amar
Robinson, Giles
Aldinger, Kimberly
Hovestadt, Volker
Tillman, Heather
Orr, Brent
Patay, Zoltán
Millen, Kathleen
Northcott, Paul
MEDB-78. Unified rhombic lip origins of Group 3 and Group 4 medulloblastoma
title MEDB-78. Unified rhombic lip origins of Group 3 and Group 4 medulloblastoma
title_full MEDB-78. Unified rhombic lip origins of Group 3 and Group 4 medulloblastoma
title_fullStr MEDB-78. Unified rhombic lip origins of Group 3 and Group 4 medulloblastoma
title_full_unstemmed MEDB-78. Unified rhombic lip origins of Group 3 and Group 4 medulloblastoma
title_short MEDB-78. Unified rhombic lip origins of Group 3 and Group 4 medulloblastoma
title_sort medb-78. unified rhombic lip origins of group 3 and group 4 medulloblastoma
topic Medulloblastoma
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9165102/
http://dx.doi.org/10.1093/neuonc/noac079.452
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