Single-cell MultiOmics and spatial transcriptomics demonstrate neuroblastoma developmental plasticity

Yunyun Xu; Daohua Lou; Ping Chen; Gang Li; Dimtry Usoskin; Jian Pan; Fang Li; Shungen Huang; Caroline Hess; Ruze Tang; Xiaohan Hu; Juanjuan Yu; Maria Arceo; Ronald R. de Krijger; Arthur S. Tischler; Susanne Schlisio; Patrik Ernfors; Yizhou Hu; Jian Wang

doi:10.1016/j.devcel.2025.04.013

Single-cell MultiOmics and spatial transcriptomics demonstrate neuroblastoma developmental plasticity

Yunyun Xu
, Daohua Lou
, Ping Chen
, Gang Li
, Dimtry Usoskin
, Jian Pan
, Fang Li
, Shungen Huang
, Caroline Hess
, Ruze Tang
, Xiaohan Hu
, Juanjuan Yu
, Maria Arceo
, Ronald R. de Krijger
, Arthur S. Tischler
, Susanne Schlisio
, Patrik Ernfors
, Yizhou Hu
, Jian Wang

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10 Citaten (Scopus)

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Neuroblastoma, the most prevalent extracranial pediatric solid tumor, arises from neural crest progeny cells. It exhibits substantial developmental plasticity and intratumoral heterogeneity, leading to survival rates below 50% in high-risk cases. The regulatory mechanisms underlying this plasticity remain largely elusive. In this integrative study, we used single-cell MultiOmics from a mouse spontaneous tumor model and spatial transcriptomics from human patient samples to dissect the transcriptional and epigenetic landscapes that govern developmental states in neuroblastoma. We identified developmental intermediate states in high-risk neuroblastomas critical for malignant transitions and uncovered extensive epigenetic priming with latent capacity for diverse state transitions. Furthermore, we mapped enhancer gene regulatory networks (eGRNs) and tumor microenvironments sustaining these aggressive states. State transitions and malignancy could be interfered with by targeting transcription factors controlling the eGRNs.

Originele taal-2	Engels
Pagina's (van-tot)	2248-2263.e11
Tijdschrift	Developmental Cell
Volume	60
Nummer van het tijdschrift	17
DOI's	https://doi.org/10.1016/j.devcel.2025.04.013
Status	Gepubliceerd - 8 sep. 2025

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10.1016/j.devcel.2025.04.013

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Xu, Y., Lou, D., Chen, P., Li, G., Usoskin, D., Pan, J., Li, F., Huang, S., Hess, C., Tang, R., Hu, X., Yu, J., Arceo, M., de Krijger, R. R., Tischler, A. S., Schlisio, S., Ernfors, P., Hu, Y., & Wang, J. (2025). Single-cell MultiOmics and spatial transcriptomics demonstrate neuroblastoma developmental plasticity. Developmental Cell, 60(17), 2248-2263.e11. https://doi.org/10.1016/j.devcel.2025.04.013

@article{996a8f4b48e24600a5dc9dc1f2836b67,

title = "Single-cell MultiOmics and spatial transcriptomics demonstrate neuroblastoma developmental plasticity",

abstract = "Neuroblastoma, the most prevalent extracranial pediatric solid tumor, arises from neural crest progeny cells. It exhibits substantial developmental plasticity and intratumoral heterogeneity, leading to survival rates below 50\% in high-risk cases. The regulatory mechanisms underlying this plasticity remain largely elusive. In this integrative study, we used single-cell MultiOmics from a mouse spontaneous tumor model and spatial transcriptomics from human patient samples to dissect the transcriptional and epigenetic landscapes that govern developmental states in neuroblastoma. We identified developmental intermediate states in high-risk neuroblastomas critical for malignant transitions and uncovered extensive epigenetic priming with latent capacity for diverse state transitions. Furthermore, we mapped enhancer gene regulatory networks (eGRNs) and tumor microenvironments sustaining these aggressive states. State transitions and malignancy could be interfered with by targeting transcription factors controlling the eGRNs.",

keywords = "development, developmental plasticity, epigenetic priming, gene regulatory network, intermediate state, intratumoral heterogeneity, microenvironment, neuroblastoma, single-cell MultiOmics, spatial transcriptomics, Single-Cell Analysis/methods, Humans, Multiomics, Gene Expression Profiling, Transcriptome/genetics, Gene Regulatory Networks/genetics, Animals, Neuroblastoma/genetics, Mice, Gene Expression Regulation, Neoplastic/genetics, Tumor Microenvironment/genetics, Epigenesis, Genetic/genetics",

author = "Yunyun Xu and Daohua Lou and Ping Chen and Gang Li and Dimtry Usoskin and Jian Pan and Fang Li and Shungen Huang and Caroline Hess and Ruze Tang and Xiaohan Hu and Juanjuan Yu and Maria Arceo and \{de Krijger\}, \{Ronald R.\} and Tischler, \{Arthur S.\} and Susanne Schlisio and Patrik Ernfors and Yizhou Hu and Jian Wang",

year = "2025",

month = sep,

day = "8",

doi = "10.1016/j.devcel.2025.04.013",

language = "English",

volume = "60",

pages = "2248--2263.e11",

journal = "Developmental Cell",

issn = "1534-5807",

publisher = "Cell Press",

number = "17",

}

Xu, Y, Lou, D, Chen, P, Li, G, Usoskin, D, Pan, J, Li, F, Huang, S, Hess, C, Tang, R, Hu, X, Yu, J, Arceo, M, de Krijger, RR, Tischler, AS, Schlisio, S, Ernfors, P, Hu, Y & Wang, J 2025, 'Single-cell MultiOmics and spatial transcriptomics demonstrate neuroblastoma developmental plasticity', Developmental Cell, vol. 60, nr. 17, blz. 2248-2263.e11. https://doi.org/10.1016/j.devcel.2025.04.013

TY - JOUR

T1 - Single-cell MultiOmics and spatial transcriptomics demonstrate neuroblastoma developmental plasticity

AU - Xu, Yunyun

AU - Lou, Daohua

AU - Chen, Ping

AU - Li, Gang

AU - Usoskin, Dimtry

AU - Pan, Jian

AU - Li, Fang

AU - Huang, Shungen

AU - Hess, Caroline

AU - Tang, Ruze

AU - Hu, Xiaohan

AU - Yu, Juanjuan

AU - Arceo, Maria

AU - de Krijger, Ronald R.

AU - Tischler, Arthur S.

AU - Schlisio, Susanne

AU - Ernfors, Patrik

AU - Hu, Yizhou

AU - Wang, Jian

PY - 2025/9/8

Y1 - 2025/9/8

N2 - Neuroblastoma, the most prevalent extracranial pediatric solid tumor, arises from neural crest progeny cells. It exhibits substantial developmental plasticity and intratumoral heterogeneity, leading to survival rates below 50% in high-risk cases. The regulatory mechanisms underlying this plasticity remain largely elusive. In this integrative study, we used single-cell MultiOmics from a mouse spontaneous tumor model and spatial transcriptomics from human patient samples to dissect the transcriptional and epigenetic landscapes that govern developmental states in neuroblastoma. We identified developmental intermediate states in high-risk neuroblastomas critical for malignant transitions and uncovered extensive epigenetic priming with latent capacity for diverse state transitions. Furthermore, we mapped enhancer gene regulatory networks (eGRNs) and tumor microenvironments sustaining these aggressive states. State transitions and malignancy could be interfered with by targeting transcription factors controlling the eGRNs.

AB - Neuroblastoma, the most prevalent extracranial pediatric solid tumor, arises from neural crest progeny cells. It exhibits substantial developmental plasticity and intratumoral heterogeneity, leading to survival rates below 50% in high-risk cases. The regulatory mechanisms underlying this plasticity remain largely elusive. In this integrative study, we used single-cell MultiOmics from a mouse spontaneous tumor model and spatial transcriptomics from human patient samples to dissect the transcriptional and epigenetic landscapes that govern developmental states in neuroblastoma. We identified developmental intermediate states in high-risk neuroblastomas critical for malignant transitions and uncovered extensive epigenetic priming with latent capacity for diverse state transitions. Furthermore, we mapped enhancer gene regulatory networks (eGRNs) and tumor microenvironments sustaining these aggressive states. State transitions and malignancy could be interfered with by targeting transcription factors controlling the eGRNs.

KW - development

KW - developmental plasticity

KW - epigenetic priming

KW - gene regulatory network

KW - intermediate state

KW - intratumoral heterogeneity

KW - microenvironment

KW - neuroblastoma

KW - single-cell MultiOmics

KW - spatial transcriptomics

KW - Single-Cell Analysis/methods

KW - Humans

KW - Multiomics

KW - Gene Expression Profiling

KW - Transcriptome/genetics

KW - Gene Regulatory Networks/genetics

KW - Animals

KW - Neuroblastoma/genetics

KW - Mice

KW - Gene Expression Regulation, Neoplastic/genetics

KW - Tumor Microenvironment/genetics

KW - Epigenesis, Genetic/genetics

UR - https://www.scopus.com/pages/publications/105004823116

UR - https://www.mendeley.com/catalogue/798e489e-4934-37ad-a8db-4ee3f2a1c95e/

U2 - 10.1016/j.devcel.2025.04.013

DO - 10.1016/j.devcel.2025.04.013

M3 - Article

C2 - 40347947

AN - SCOPUS:105004823116

SN - 1534-5807

VL - 60

SP - 2248-2263.e11

JO - Developmental Cell

JF - Developmental Cell

IS - 17

ER -

Single-cell MultiOmics and spatial transcriptomics demonstrate neuroblastoma developmental plasticity

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