AI Article Synopsis

  • Neuroblastoma differentiation is key for treatment but not well understood; researchers created a computational model revealing gene clusters linked to this process.
  • They identified a differentiation signature with 1,251 genes that can predict outcomes in patients and are influenced by MYCN expression.
  • The study highlights the value of using Boolean network analysis to discover new genes and pathways, including the role of UBE4B, which could be potential targets for neuroblastoma therapy.

Article Abstract

Although induction of differentiation represents an effective strategy for neuroblastoma treatment, the mechanisms underlying neuroblastoma differentiation are poorly understood. We generated a computational model of neuroblastoma differentiation consisting of interconnected gene clusters identified based on symmetric and asymmetric gene expression relationships. We identified a differentiation signature consisting of series of gene clusters comprised of 1251 independent genes that predicted neuroblastoma differentiation in independent datasets and in neuroblastoma cell lines treated with agents known to induce differentiation. This differentiation signature was associated with patient outcomes in multiple independent patient cohorts and validated the role of MYCN expression as a marker of neuroblastoma differentiation. Our results further identified novel genes associated with MYCN via asymmetric Boolean implication relationships that would not have been identified using symmetric computational approaches and that were associated with both neuroblastoma differentiation and patient outcomes. Our differentiation signature included a cluster of genes involved in intracellular signaling and growth factor receptor trafficking pathways that is strongly associated with neuroblastoma differentiation, and we validated the associations of UBE4B, a gene within this cluster, with neuroblastoma cell and tumor differentiation. Our findings demonstrate that Boolean network analyses of symmetric and asymmetric gene expression relationships can identify novel genes and pathways relevant for neuroblastoma tumor differentiation that could represent potential therapeutic targets.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10257350PMC
http://dx.doi.org/10.1002/gcc.23124DOI Listing

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