p16 Loss and E2F/cell cycle deregulation in infant posterior fossa ependymoma.
Seth C LummusAndrew M DonsonKatherine GowanKenneth L JonesRajeev VibhakarNicholas K ForemanBette K Kleinschmidt-DeMastersPublished in: Pediatric blood & cancer (2017)
Biological differences, characterized by loss of p16 expression without gains of 1q in iEPN-PFs, as well as deregulated E2F target gene transcription, are indicative of deregulated p16-CDK4/6-pRB-E2F pathway activity. This may underlie the poor clinical outcome seen in this group of iEPN-PFs, rather than the withholding of radiation therapy. Results suggest a potential actionable therapy for iEPN-PF, namely cyclin-dependent kinase 4/6 (CDK4/6) inhibitors.