MBRS-57. IDENTIFICATION OF MYC-DEPENDENT THERAPEUTIC VULNERABILITIES FOR TARGETING GROUP 3 MEDULLOBLASTOMA

Group 3 medulloblastoma (MB(Group3)) is a highly aggressive tumour characterised by MYC amplification and elevated expression (17% of MB(Group3)). MYC amplification in MB(Group3) confers a dismal prognosis using standard therapies, and there is an urgent unmet need for novel therapeutic approaches....

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Detalles Bibliográficos
Autores principales: Llargués-Sistac, Gemma, Lindsey, Janet, Swartz, Shanel, Selby, Matthew, Morcavallo, Alaide, Bailey, Simon, Chesler, Louis, Lord, Christopher J, Williamson, Daniel, Clifford, Steven C
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2020
Materias:
Medulloblastoma (Research)
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7715234/
http://dx.doi.org/10.1093/neuonc/noaa222.562
Descripción
Sumario:Group 3 medulloblastoma (MB(Group3)) is a highly aggressive tumour characterised by MYC amplification and elevated expression (17% of MB(Group3)). MYC amplification in MB(Group3) confers a dismal prognosis using standard therapies, and there is an urgent unmet need for novel therapeutic approaches. The identification and targeting of MYC’s biological dependencies thus represents a promising strategy to treat MYC-MB(Group3) tumours. Three independent isogenic MYC-regulable MB(Group3) human cell-based models, in which elevated MYC expression can be directly down-regulated by doxycycline-inducible shRNAs, were developed and used initially to establish MYC-dependent growth of each model. Our novel models were then used to investigate MYC-dependent drug sensitivity, by characterising responses to a panel of candidate cancer therapeutics and small molecule inhibitors, including a high-throughput compound screen of >500 established/clinically-relevant small molecule inhibitors. This approach identified several specific, consistently observed, druggable MYC-dependencies (e.g. cell cycle regulators, DNA-damage response controllers, mitotic control machinery) with potential for the development of treatments against MYC-MB(Group3) tumours. PLK1, CHK1 and AURK were identified as prime candidate targets with consistent MYC-dependent response profiles. Subsequent validation of each candidate, by genetic and pharmacological target inhibition, confirmed their MYC-dependent effects, associated with downregulation of MYC and established target-dependent pharmacodynamic biomarkers/pathways. Results were consistent across all of our MB(Group3) models. In summary, our novel models reveal druggable MYC-associated dependencies as a feature of MB(Group3.) Our findings support the development of PLK1, CHK1 and AURK inhibition as therapeutic approaches against MYC-dependent MB(Group3). Future work is now essential to validate our findings in vivo, to support the design of future clinical trials.

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