Abstract
BackgroundThrough negative regulation of gene expression, microRNAs (miRNAs) can function as oncosuppressors in cancers, and can themselves show altered expression in various tumor types. Here, we have investigated medulloblastoma tumors (MBs), which arise from an early impairment of developmental processes in the cerebellum, where Notch signaling is involved in many of the cell-fate-determining stages. Notch regulates a subset of MB cells that have stem-cell-like properties and can promote tumor growth. On the basis of this evidence, we hypothesized that miRNAs targeting the Notch pathway can regulate these phenomena, and can be used in anti-cancer therapies.Methodology/Principal FindingsIn a screening of potential targets within Notch signaling, miR-34a was seen to be a regulator of the Notch pathway through its targeting of Notch ligand Delta-like 1 (Dll1). Down-regulation of Dll1 expression by miR-34a negatively regulates cell proliferation, and induces apoptosis and neural differentiation in MB cells. Using an inducible tetracycline on-off model of miR-34a expression, we show that in Daoy MB cells, Dll1 is the first target that is regulated in MB, as compared to the other targets analyzed here: Cyclin D1, cMyc and CDK4. MiR-34a expression negatively affects CD133+/CD15+ tumor-propagating cells, then we assay through reverse-phase proteomic arrays, Akt and Stat3 signaling hypo-phosphorylation. Adenoviruses carrying the precursor miR-34a induce neurogenesis of tumor spheres derived from a genetic animal model of MB (Patch1+/- p53-/-), thus providing further evidence that the miR-34a/Dll1 axis controls both autonomous and non autonomous signaling of Notch. In vivo, miR-34a overexpression carried by adenoviruses reduces tumor burden in cerebellum xenografts of athymic mice, thus demonstrating an anti-tumorigenic role of miR-34a in vivo.Conclusions/SignificanceDespite advances in our understanding of the pathogenesis of MB, one-third of patients with MB remain incurable. Here, we show that stable nucleic-acid-lipid particles carrying mature miR-34a can target Dll1 in vitro and show equal effects to those of adenovirus miR-34a cell infection. Thus, this technology forms the basis for their therapeutic use for the delivery of miR-34a in brain-tumor treatment, with no signs of toxicity described to date in non-human primate trials.
Highlights
Medulloblastoma (MB) is the most common malignant and highly invasive embryonal tumor in children
We investigated whether miR-34a was able to influences both Notch 1 and Notch2 receptor signaling in medulloblastoma tumors (MBs) cells through its down-regulation of Delta-like 1 (Dll1), considering both cell autonomous and non-autonomous [27,28]
We have shown that miR-34a targets Notch ligand Dll1 in MB cell lines
Summary
Medulloblastoma (MB) is the most common malignant and highly invasive embryonal tumor in children It originates in the cerebellum, and accounts for more than 25% of childhood cancer-related deaths [1]. MB can arise from granule-cell progenitors and neural stem cells (NSCs) of the cerebellum [2]. Pathways such as Notch and Sonic Hedgehog (Shh), which control cerebellum development, are crucially involved in MB tumorigenesis [3,4]. MiR-199b-5p regulates the Hes gene, a key effector of the Notch pathway, and inhibits proliferation and survival of MB CD133+ cancer-stem-cell populations. We have investigated medulloblastoma tumors (MBs), which arise from an early impairment of developmental processes in the cerebellum, where Notch signaling is involved in many of the cell-fate-determining stages. On the basis of this evidence, we hypothesized that miRNAs targeting the Notch pathway can regulate these phenomena, and can be used in anti-cancer therapies
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