AI Article Synopsis
- Chemotherapy resistance is a significant factor contributing to high mortality rates in neuroblastoma, particularly in tumors with MYCN amplification.
- Researchers developed an embryonic stem cell (ESC) miRNA and mRNA signature to identify neuroblastomas with high pluripotency, which are linked to worse patient outcomes.
- The study also found that FOXM1 is a crucial driver of this ESC signature, suggesting that targeting FOXM1 in drug design could potentially improve therapy effectiveness against resistant neuroblastomas.
Article Abstract
Chemotherapy resistance is responsible for high mortality rates in neuroblastoma. MYCN, an oncogenic driver in neuroblastoma, controls pluripotency genes including LIN28B. We hypothesized that enhanced embryonic stem cell (ESC) gene regulatory programs could mark tumors with high pluripotency capacity and subsequently increased risk for therapy failure. An ESC miRNA signature was established based on publicly available data. In addition, an ESC mRNA signature was generated including the 500 protein coding genes with the highest positive expression correlation with the ESC miRNA signature score in 200 neuroblastomas. High ESC m(i)RNA expression signature scores were significantly correlated with poor neuroblastoma patient outcome specifically in the subgroup of MYCN amplified tumors and stage 4 nonamplified tumors. Further data-mining identified FOXM1, as the major predicted driver of this ESC signature, controlling a large set of genes implicated in cell cycle control and DNA damage response. Of further interest, re-analysis of published data showed that MYCN transcriptionally activates FOXM1 in neuroblastoma cells. In conclusion, a novel ESC m(i)RNA signature stratifies neuroblastomas with poor prognosis, enabling the identification of therapy-resistant tumors. The finding that this signature is strongly FOXM1 driven, warrants for drug design targeted at FOXM1 or key components controlling this pathway.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6269481 | PMC |
| http://dx.doi.org/10.1038/s41598-018-35868-5 | DOI Listing |
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