AI Article Synopsis

  • - Neuroblastoma (NB) is a serious and complex childhood cancer that can vary widely in its progression; while some tumors may shrink on their own or respond to treatment, about 40% of patients face severe outcomes, especially those in the high-risk category.
  • - Researchers used advanced techniques, like single-cell multi-omics and sequencing, to study human NB and discovered not only adrenergic tumor cells but also unique, aneuploid SCP-like cells that exhibit clonal expansion and specific gene expression patterns.
  • - The study suggests that aneuploid SCP-like cells are a new aspect of NB, indicating that these cells, which may arise from the neural crest lineage, could play a key role in the early

Article Abstract

Background: Neuroblastoma (NB) is a heterogeneous embryonal malignancy and the deadliest tumor of infancy. It is a complex disease that can result in diverse clinical outcomes. In some children, tumors regress spontaneously. Others respond well to existing treatments. But for the high-risk group, which constitutes approximately 40% of all patients, the prognosis remains dire despite collaborative efforts in basic and clinical research. While its exact cellular origin is still under debate, NB is assumed to arise from the neural crest cell lineage including multipotent Schwann cell precursors (SCPs), which differentiate into sympatho-adrenal cell states eventually producing chromaffin cells and sympathoblasts.

Methods: To investigate clonal development of neuroblastoma cell states, we performed haplotype-specific analysis of human tumor samples using single-cell multi-omics, including joint DNA/RNA sequencing of sorted single cells (DNTR-seq). Samples were also assessed using immunofluorescence stainings and fluorescence in-situ hybridization (FISH).

Results: Beyond adrenergic tumor cells, we identify subpopulations of aneuploid SCP-like cells, characterized by clonal expansion, whole-chromosome 17 gains, as well as expression programs of proliferation, apoptosis, and a non-immunomodulatory phenotype.

Conclusion: Aneuploid pre-malignant SCP-like cells represent a novel feature of NB. Genetic evidence and tumor phylogeny suggest that these clones and malignant adrenergic populations originate from aneuploidy-prone cells of migrating neural crest or SCP origin, before lineage commitment to sympatho-adrenal cell states. Our findings expand the phenotypic spectrum of NB cell states. Considering the multipotency of SCPs in development, we suggest that the transformation of fetal SCPs may represent one possible mechanism of tumor initiation in NB with chromosome 17 aberrations as a characteristic element.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11365129PMC
http://dx.doi.org/10.1186/s12943-024-02091-yDOI Listing

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