Mesenchymal and adrenergic cell lineage states in neuroblastoma possess distinct immunogenic phenotypes
Publication date
2022-10
Authors
Sengupta, Satyaki
Das, Sanjukta
Crespo, Angela C
Cornel, Annelisa M.
Patel, Anand G
Mahadevan, Navin R
Campisi, Marco
Ali, Alaa K
Sharma, Bandana
Rowe, Jared H
Editors
Advisors
Supervisors
Document Type
Article
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taverne
Abstract
Apart from the anti-GD2 antibody, immunotherapy for neuroblastoma has had limited success due to immune evasion mechanisms, coupled with an incomplete understanding of predictors of response. Here, from bulk and single-cell transcriptomic analyses, we identify a subset of neuroblastomas enriched for transcripts associated with immune activation and inhibition and show that these are predominantly characterized by gene expression signatures of the mesenchymal lineage state. By contrast, tumors expressing adrenergic lineage signatures are less immunogenic. The inherent presence or induction of the mesenchymal state through transcriptional reprogramming or therapy resistance is accompanied by innate and adaptive immune gene activation through epigenetic remodeling. Mesenchymal lineage cells promote T cell infiltration by secreting inflammatory cytokines, are efficiently targeted by cytotoxic T and natural killer cells and respond to immune checkpoint blockade. Together, we demonstrate that distinct immunogenic phenotypes define the divergent lineage states of neuroblastoma and highlight the immunogenic potential of the mesenchymal lineage.
Keywords
Taverne, Oncology, Cancer Research, Journal Article
Citation
Sengupta, S, Das, S, Crespo, A C, Cornel, A M, Patel, A G, Mahadevan, N R, Campisi, M, Ali, A K, Sharma, B, Rowe, J H, Huang, H, Debruyne, D N, Cerda, E D, Krajewska, M, Dries, R, Chen, M, Zhang, S, Soriano, L, Cohen, M A, Versteeg, R, Jaenisch, R, Spranger, S, Romee, R, Miller, B C, Barbie, D A, Nierkens, S, Dyer, M A, Lieberman, J & George, R E 2022, 'Mesenchymal and adrenergic cell lineage states in neuroblastoma possess distinct immunogenic phenotypes', Nature Cancer, vol. 3, no. 10, pp. 1228-1246. https://doi.org/10.1038/s43018-022-00427-5