Abstract
Simple SummaryNeuroblastoma is a tumor of the sympathetic nervous system that substantially contributes to childhood cancer mortality. Neuroblastoma originates from the neural crest cells that are subjected to genetic alterations during embryonic development. These impairments hit key genes, whose expression is activated/repressed by transcription factors and inhibited by negative regulators, named microRNAs, thereby promoting tumorigenesis. Here, we have focused on the interactions between the transcription factors MYCN and PHOX2B with their target genes ALK and LIN28B and the miRNAs let-7, miR-34 and miR-204, which should act as negative regulators of their expression. In neuroblastoma, the physiologic regulatory networks among these genes and microRNAs are disrupted, leading to a complex and aberrant oncogene expression that underlies the development of the tumor. We also looked into the role of these genetic determinants of neuroblastoma starting from their physiological role in neural crest development and ending with their pathogenic dysregulation that leads to neuroblastoma oncogenesis.Neuroblastoma (NB) is a tumor of the peripheral sympathetic nervous system that substantially contributes to childhood cancer mortality. NB originates from neural crest cells (NCCs) undergoing a defective sympathetic neuronal differentiation and although the starting events leading to the development of NB remain to be fully elucidated, the master role of genetic alterations in key oncogenes has been ascertained: (1) amplification and/or over-expression of MYCN, which is strongly associated with tumor progression and invasion; (2) activating mutations, amplification and/or over-expression of ALK, which is involved in tumor initiation, angiogenesis and invasion; (3) amplification and/or over-expression of LIN28B, promoting proliferation and suppression of neuroblast differentiation; (4) mutations and/or over-expression of PHOX2B, which is involved in the regulation of NB differentiation, stemness maintenance, migration and metastasis. Moreover, altered microRNA (miRNA) expression takes part in generating pathogenetic networks, in which the regulatory loops among transcription factors, miRNAs and target genes lead to complex and aberrant oncogene expression that underlies the development of a tumor. In this review, we have focused on the circuitry linking the oncogenic transcription factors MYCN and PHOX2B with their transcriptional targets ALK and LIN28B and the tumor suppressor microRNAs let-7, miR-34 and miR-204, which should act as down-regulators of their expression. We have also looked at the physiologic role of these genetic and epigenetic determinants in NC development, as well as in terminal differentiation, with their pathogenic dysregulation leading to NB oncogenesis.
Highlights
Current address: Unità Operativa Proteomica e Spettrometria di Massa, IRCCS Ospedale Policlinico San Martino, 16132 Genoa, Italy
The role of tumor suppressor (TS) miRNAs is relevant, whose involvement in NB development is well documented. Among these numerous TS miRNAs, we have focused on let-7 [18,20,21,33], miR-34 [34,35,36,37] and miR-204 [38,39,40], which physiologically act as down-regulators of MYCN and paired-like homeobox 2B (PHOX2B) and their targets Anaplastic lymphoma kinase (ALK) and LIN28B
We have focused on the regulatory circuitry linking TS miRNAs let‐7, loops (Figure 3) that are disrupted in NB, thereby generating a loss of inhibitory functions miR‐34 and miR‐204 with the oncogenic transcription factors (TFs) MYCN and PHOX2B and their transcrip‐
Summary
Neuroblastoma (NB) is a pediatric tumor originating from neural crest (NC)-derived cells subjected to defective differentiation due to genomic and epigenetic impairments. As most primary NB tumors arise from the AM, investigations on the potential cell population involved in NB development have mainly been focused on the embryonic adrenal development These observations have disclosed the specific NC-derived cell populations that may undergo impairments at genetic/epigenetic determinants that control the NB gene expression programs, thereby promoting tumorigenesis. ADRN and MES cell types can spontaneously interconvert into each other by altering their transcriptional states through an epigenetic mechanism of reprogramming [41,42] that confers high plasticity to NB Another important aspect emerging from these studies is the discovery of two superenhancers (SEs) and associated lineage-specific transcription factors (TFs) that form specific core regulatory circuitries (CRC) (see below) and underlie MES and ADRN cell identity states. The MES-specific CRC includes the TFs PRRX1, TWIST1, SNAI2 and MAML3; NOTCH members RUNX1, NFKB and AP-1; TF family members (including JUN and FOS family members), the retinoic acid receptor beta RARB and many others [41,42,50,52,55]
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