A spatial cell atlas of neuroblastoma reveals developmental, epigenetic and spatial axis of tumor he...
A spatial cell atlas of neuroblastoma reveals developmental, epigenetic and spatial axis of tumor heterogeneity
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Author / Creator
Patel, Anand G , Ashenberg, Orr , Collins, Natalie B , Segerstolpe, Åsa , Jiang, Sizun , Slyper, Michal , Huang, Xin , Caraccio, Chiara , Jin, Hongjian , Sheppard, Heather , Xu, Ke , Chang, Ti-Cheng , Orr, Brent A , Shirinifard, Abbas , Chapple, Richard H , Shen, Amber , Clay, Michael R , Tatevossian, Ruth G , Reilly, Colleen , Patel, Jaimin , Lupo, Marybeth , Cline, Cynthia , Dionne, Danielle , Porter, Caroline B M , Waldman, Julia , Bai, Yunhao , Zhu, Bokai , Barrera, Irving , Murray, Evan , Vigneau, Sébastien , Napolitano, Sara , Wakiro, Isaac , Wu, Jingyi , Grimaldi, Grace , Dellostritto, Laura , Helvie, Karla , Rotem, Asaf , Lako, Ana , Cullen, Nicole , Pfaff, Kathleen L , Karlström, Åsa , Jané-Valbuena, Judit , Todres, Ellen , Thorner, Aaron , Geeleher, Paul , Rodig, Scott J , Zhou, Xin , Stewart, Elizabeth , Johnson, Bruce E , Wu, Gang , Chen, Fei , Yu, Jiyang , Goltsev, Yury , Nolan, Garry P , Rozenblatt-Rosen, Orit , Regev, Aviv and Dyer, Michael A
Publisher
United States: Cold Spring Harbor Laboratory Press
Journal title
Language
English
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Publisher
United States: Cold Spring Harbor Laboratory Press
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Scope and Contents
Contents
Neuroblastoma is a pediatric cancer arising from the developing sympathoadrenal lineage with complex inter- and intra-tumoral heterogeneity. To chart this complexity, we generated a comprehensive cell atlas of 55 neuroblastoma patient tumors, collected from two pediatric cancer institutions, spanning a range of clinical, genetic, and histologic features. Our atlas combines single-cell/nucleus RNA-seq (sc/scRNA-seq), bulk RNA-seq, whole exome sequencing, DNA methylation profiling, spatial transcriptomics, and two spatial proteomic methods. Sc/snRNA-seq revealed three malignant cell states with features of sympathoadrenal lineage development. All of the neuroblastomas had malignant cells that resembled sympathoblasts and the more differentiated adrenergic cells. A subset of tumors had malignant cells in a mesenchymal cell state with molecular features of Schwann cell precursors. DNA methylation profiles defined four groupings of patients, which differ in the degree of malignant cell heterogeneity and clinical outcomes. Using spatial proteomics, we found that neuroblastomas are spatially compartmentalized, with malignant tumor cells sequestered away from immune cells. Finally, we identify spatially restricted signaling patterns in immune cells from spatial transcriptomics. To facilitate the visualization and analysis of our atlas as a resource for further research in neuroblastoma, single cell, and spatial-omics, all data are shared through the Human Tumor Atlas Network Data Commons at www.humantumoratlas.org....
Alternative Titles
Full title
A spatial cell atlas of neuroblastoma reveals developmental, epigenetic and spatial axis of tumor heterogeneity
Authors, Artists and Contributors
Author / Creator
Ashenberg, Orr
Collins, Natalie B
Segerstolpe, Åsa
Jiang, Sizun
Slyper, Michal
Huang, Xin
Caraccio, Chiara
Jin, Hongjian
Sheppard, Heather
Xu, Ke
Chang, Ti-Cheng
Orr, Brent A
Shirinifard, Abbas
Chapple, Richard H
Shen, Amber
Clay, Michael R
Tatevossian, Ruth G
Reilly, Colleen
Patel, Jaimin
Lupo, Marybeth
Cline, Cynthia
Dionne, Danielle
Porter, Caroline B M
Waldman, Julia
Bai, Yunhao
Zhu, Bokai
Barrera, Irving
Murray, Evan
Vigneau, Sébastien
Napolitano, Sara
Wakiro, Isaac
Wu, Jingyi
Grimaldi, Grace
Dellostritto, Laura
Helvie, Karla
Rotem, Asaf
Lako, Ana
Cullen, Nicole
Pfaff, Kathleen L
Karlström, Åsa
Jané-Valbuena, Judit
Todres, Ellen
Thorner, Aaron
Geeleher, Paul
Rodig, Scott J
Zhou, Xin
Stewart, Elizabeth
Johnson, Bruce E
Wu, Gang
Chen, Fei
Yu, Jiyang
Goltsev, Yury
Nolan, Garry P
Rozenblatt-Rosen, Orit
Regev, Aviv
Dyer, Michael A
Identifiers
Primary Identifiers
Record Identifier
TN_cdi_proquest_journals_2911043327
Permalink
https://devfeature-collection.sl.nsw.gov.au/record/TN_cdi_proquest_journals_2911043327
Other Identifiers
ISSN
2692-8205
E-ISSN
2692-8205
DOI
10.1101/2024.01.07.574538