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Molecular and clinical heterogeneity within <i>MYC</i>-family amplified medulloblastoma is associated with survival outcomes: A multicenter cohort study

DOIFull Paper Access

18

Citations

32

References

2024

Year

Ed C. Schwalbe, Janet C. Lindsey, Marina Danilenko, Rebecca M. Hill, Stephen Crosier, Sarra Ryan, Daniel Williamson, Jemma Castle, Debbie Hicks, Marcel Kool,
Neuro-Oncology

Abstract

MYC(N)-amplified MB displays significant clinicobiological heterogeneity. Diagnostics incorporating molecular groups, subgroups, and clinical factors enable their risk assessment. VHR "canonical" MYC tumors are essentially incurable and SHH-MYCN-amplified MBs fare extremely poorly (20% survival at 5 years); both require urgent development of alternative treatment strategies. Conventional risk-adapted therapies are appropriate for more responsive groups, such as noncanonical MYC and non-SHH-MYCN MB.

References

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