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Resolving Medulloblastoma Cellular Architecture by Single-cell Genomics

Overview
Journal Nature
Specialty Science
Date 2019 Jul 26
PMID 31341285
Citations 191
Authors
Volker Hovestadt
Kyle S Smith
Laure Bihannic
Mariella G Filbin
McKenzie L Shaw
Alicia Baumgartner
John C DeWitt
Andrew Groves
Lisa Mayr
Hannah R Weisman
Alyssa R Richman
Marni E Shore
Liliana Goumnerova
Celeste Rosencrance
Robert A Carter
Timothy N Phoenix
Jennifer L Hadley
Yiai Tong
Jim Houston
Richard A Ashmun
Michael DeCuypere
Tanvi Sharma
Diane Flasch
Antonina Silkov
Keith L Ligon
Scott L Pomeroy
Miguel N Rivera
Orit Rozenblatt-Rosen
Jessica M Rusert
Robert J Wechsler-Reya
Xiao-Nan Li
Andreas Peyrl
Johannes Gojo
Dominik Kirchhofer
Daniela Lotsch
Thomas Czech
Christian Dorfer
Christine Haberler
Rene Geyeregger
Angela Halfmann
Charles Gawad
John Easton
Stefan M Pfister
Aviv Regev
Amar Gajjar
Brent A Orr
Irene Slavc
Giles W Robinson
Bradley E Bernstein
Mario L Suva
Paul A Northcott
Affiliations
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Abstract

Medulloblastoma is a malignant childhood cerebellar tumour type that comprises distinct molecular subgroups. Whereas genomic characteristics of these subgroups are well defined, the extent to which cellular diversity underlies their divergent biology and clinical behaviour remains largely unexplored. Here we used single-cell transcriptomics to investigate intra- and intertumoral heterogeneity in 25 medulloblastomas spanning all molecular subgroups. WNT, SHH and Group 3 tumours comprised subgroup-specific undifferentiated and differentiated neuronal-like malignant populations, whereas Group 4 tumours consisted exclusively of differentiated neuronal-like neoplastic cells. SHH tumours closely resembled granule neurons of varying differentiation states that correlated with patient age. Group 3 and Group 4 tumours exhibited a developmental trajectory from primitive progenitor-like to more mature neuronal-like cells, the relative proportions of which distinguished these subgroups. Cross-species transcriptomics defined distinct glutamatergic populations as putative cells-of-origin for SHH and Group 4 subtypes. Collectively, these data provide insights into the cellular and developmental states underlying subtype-specific medulloblastoma biology.

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