Adrenergic and mesenchymal signatures are identifiable in cell‐free DNA and correlate with metastatic disease burden in children with neuroblastoma

Vayani, Omar R.; Kaufman, Maria E.; Moore, Kelley; Chennakesavalu, Mohansrinivas; TerHaar, Rachel; Chaves, Gepoliano; Chlenski, Alexandre; He, Chuan; Cohn, Susan L.; Applebaum, Mark A.

doi:10.1002/pbc.30735

Cited by 4 publications

(1 citation statement)

References 63 publications

(113 reference statements)

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“…In addition, the samples could activate T cells (CD247, CD3D, CD3E, and CD3G) and B cells (CD19, SYK, BTK, and BLNK) and express signatures associated with immunotherapy. The idea that NB is unlikely to be classified as a nonimmunogenic and/or "cold" tumor, and that it is only a stage-related disease at the time of diagnosis, is supported by the gene signals automatically retrieved from the existing NB data [54]. Numerous genes involved in inflammation, mediated by the integrin signaling pathway and the chemokine and cytokine signaling pathway, also characterize the MES phenotype, whose responses are strongly triggered by cues from T-and B-lymphocyte infiltrating cells associated with a significant inflammatory state.…”

Section: Discussionmentioning

confidence: 99%

Review of Patient Gene Profiles Obtained through a Non-Negative Matrix Factorization-Based Framework to Determine the Role Inflammation Plays in Neuroblastoma Pathogenesis

Boccarelli,

Del Buono,

Esposito

2024

IJMS

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Neuroblastoma is the most common extracranial solid tumor in children. It is a highly heterogeneous tumor consisting of different subcellular types and genetic abnormalities. Literature data confirm the biological and clinical complexity of this cancer, which requires a wider availability of gene targets for the implementation of personalized therapy. This paper presents a study of neuroblastoma samples from primary tumors of untreated patients. The focus of this analysis is to evaluate the impact that the inflammatory process may have on the pathogenesis of neuroblastoma. Eighty-eight gene profiles were selected and analyzed using a non-negative matrix factorization framework to extract a subset of genes relevant to the identification of an inflammatory phenotype, whose targets (PIK3CG, NFATC2, PIK3R2, VAV1, RAC2, COL6A2, COL6A3, COL12A1, COL14A1, ITGAL, ITGB7, FOS, PTGS2, PTPRC, ITPR3) allow further investigation. Based on the genetic signals automatically derived from the data used, neuroblastoma could be classified according to stage rather than as a “cold” or “poorly immunogenic” tumor.

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Section: Discussionmentioning

confidence: 99%

Review of Patient Gene Profiles Obtained through a Non-Negative Matrix Factorization-Based Framework to Determine the Role Inflammation Plays in Neuroblastoma Pathogenesis

Boccarelli,

Del Buono,

Esposito

2024

IJMS

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Epithelial to Mesenchymal Transition in Neuroblastoma: Mechanisms and Therapeutic Considerations

Jahangiri

2024

Curr. Tissue Microenviron. Rep.

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Purpose of Review Neuroblastoma (NB) is a solid tumour of the extracranial region in children, and it originates from the developing sympathetic nervous system. Metastasis is present in circa 70% of NB cases at the time of diagnosis and may be accompanied by poor prognosis and resistance to treatment. As such, metastasis is an important step in NB progression and is the main cause of fatality in this cancer. Furthermore, metastasis is linked to epithelial to mesenchymal transition (EMT). Recent Findings EMT is characterised by the loss of the stationary compact epithelial cell arrangement and increased motility and invasion of these cells and may also be associated with patient outcomes, including treatment resistance, recurrence, and poor survival. Summary This study aims to gain mechanistic insight into EMT and review signalling pathways, proteins, non-coding RNA, and microenvironmental factors that may contribute to this process in NB. Further, drug compounds that affect EMT in NB, and proteins and non-coding RNA that impact EMT and treatment resistance will be reviewed. A better comprehension of EMT in NB will deepen our understanding of this cancer and provide new avenues for clinical interventions and therapeutic gain.

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A human neural crest model reveals the developmental impact of neuroblastoma-associated chromosomal aberrations

Saldana-Guerrero,

Montano-Gutierrez,

Boswell

et al. 2024

Nat Commun

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Early childhood tumours arise from transformed embryonic cells, which often carry large copy number alterations (CNA). However, it remains unclear how CNAs contribute to embryonic tumourigenesis due to a lack of suitable models. Here we employ female human embryonic stem cell (hESC) differentiation and single-cell transcriptome and epigenome analysis to assess the effects of chromosome 17q/1q gains, which are prevalent in the embryonal tumour neuroblastoma (NB). We show that CNAs impair the specification of trunk neural crest (NC) cells and their sympathoadrenal derivatives, the putative cells-of-origin of NB. This effect is exacerbated upon overexpression of MYCN, whose amplification co-occurs with CNAs in NB. Moreover, CNAs potentiate the pro-tumourigenic effects of MYCN and mutant NC cells resemble NB cells in tumours. These changes correlate with a stepwise aberration of developmental transcription factor networks. Together, our results sketch a mechanistic framework for the CNA-driven initiation of embryonal tumours.

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Adrenergic and mesenchymal signatures are identifiable in cell‐free DNA and correlate with metastatic disease burden in children with neuroblastoma

Cited by 4 publications

References 63 publications

Review of Patient Gene Profiles Obtained through a Non-Negative Matrix Factorization-Based Framework to Determine the Role Inflammation Plays in Neuroblastoma Pathogenesis

Review of Patient Gene Profiles Obtained through a Non-Negative Matrix Factorization-Based Framework to Determine the Role Inflammation Plays in Neuroblastoma Pathogenesis

Epithelial to Mesenchymal Transition in Neuroblastoma: Mechanisms and Therapeutic Considerations

A human neural crest model reveals the developmental impact of neuroblastoma-associated chromosomal aberrations

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