| Literature DB >> 22723427 |
Arend H Sikkema1, Wilfred F A den Dunnen, Esther Hulleman, Dannis G van Vuurden, Guillermo Garcia-Manero, Hui Yang, Frank J G Scherpen, Kim R Kampen, Eelco W Hoving, Willem A Kamps, Sander H Diks, Maikel P Peppelenbosch, Eveline S J M de Bont.
Abstract
Eph/ephrin signaling has been implicated in various types of key cancer-enhancing processes, like migration, proliferation, and angiogenesis. In medulloblastoma, invading tumor cells characteristically lead to early recurrence and a decreased prognosis. Based on kinase-activity profiling data published recently, we hypothesized a key role for the Eph/ephrin signaling system in medulloblastoma invasion. In primary medulloblastoma samples, a significantly higher expression of EphB2 and the ligand ephrin-B1 was observed compared with normal cerebellum. Furthermore, medulloblastoma cell lines showed high expression of EphA2, EphB2, and EphB4. Stimulation of medulloblastoma cells with ephrin-B1 resulted in a marked decrease in in vitro cell adhesion and an increase in the invasion capacity of cells expressing high levels of EphB2. The cell lines that showed an ephrin-B1-induced phenotype possessed increased levels of phosphorylated EphB2 and, to a lesser extent, EphB4 after stimulation. Knockdown of EphB2 expression by short hairpin RNA completely abolished ephrin ligand-induced effects on adhesion and migration. Analysis of signal transduction identified p38, Erk, and mTOR as downstream signaling mediators potentially inducing the ephrin-B1 phenotype. In conclusion, the observed deregulation of Eph/ephrin expression in medulloblastoma enhances the invasive phenotype, suggesting a potential role in local tumor cell invasion and the formation of metastases.Entities:
Mesh:
Substances:
Year: 2012 PMID: 22723427 PMCID: PMC3424207 DOI: 10.1093/neuonc/nos130
Source DB: PubMed Journal: Neuro Oncol ISSN: 1522-8517 Impact factor: 12.300