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AKT signalling is required for ribosomal RNA synthesis and progression of Eμ-Myc B-cell lymphoma in vivo

dc.contributor.authorDevlin, Jennifer
dc.contributor.authorHannan, Katherine
dc.contributor.authorNg, Pui Y.
dc.contributor.authorBywater, Megan J.
dc.contributor.authorShortt, Jake
dc.contributor.authorCullinane, C
dc.contributor.authorMcArthur, Grant
dc.contributor.authorJohnstone, Ricky
dc.contributor.authorHannan, Ross
dc.contributor.authorPearson, Richard B
dc.date.accessioned2016-06-14T23:18:40Z
dc.date.issued2013
dc.date.updated2016-06-14T08:27:57Z
dc.description.abstractThe dysregulation of PI3K/AKT/mTORC1 signalling and/or hyperactivation of MYC are observed in a high proportion of human cancers, and together they form a 'super signalling' network mediating malignancy. A fundamental downstream action of this signalling network is up-regulation of ribosome biogenesis and subsequent alterations in the patterns of translation and increased protein synthesis, which are thought to be critical for AKT/MYC-driven oncogenesis. We have demonstrated that AKT and MYC cooperate to drive ribosomal DNA (rDNA) transcription and ribosome biogenesis, with AKT being essential for rDNA transcription and in vitro survival of lymphoma cells isolated from a MYC-driven model of B-cell lymphoma (Eμ-Myc) [Chan JC et al., (2011) Science Signalling 4, ra56]. Here we show that the allosteric AKT inhibitor MK-2206 rapidly and potently antagonizes rDNA transcription in Eμ-Myc B-cell lymphomas in vivo, and this is associated with a rapid reduction in indicators of disease burden, including spleen weight and the abundance of tumour cells in both the circulation and lymph nodes. Extended treatment of tumour-bearing mice with MK-2206 resulted in a significant delay in disease progression, associated with increased B-cell lymphoma apoptosis. Our findings suggest that malignant diseases characterized by unrestrained ribosome biogenesis may be vulnerable to therapeutic strategies that target the PI3K/AKT/mTORC1/MYC growth control network. Hyperactivation of PI3K/AKT and/or MYC signalling activity is observed in many cancers and results in increased ribosome biogenesis thought to be critical for oncogenesis. We show that AKT inhibition antagonizes rDNA transcription in Eμ-Myc lymphoma and this is associated with delayed disease progression in vivo. Thus cancers characterized by unrestrained ribosome biogenesis may be vulnerable to therapies targeting PI3K/AKT signalling.
dc.identifier.issn1742-464X
dc.identifier.urihttp://hdl.handle.net/1885/102571
dc.publisherBlackwell Publishing Ltd
dc.sourceThe FEBS Journal
dc.titleAKT signalling is required for ribosomal RNA synthesis and progression of Eμ-Myc B-cell lymphoma in vivo
dc.typeJournal article
local.bibliographicCitation.issue21
local.bibliographicCitation.lastpage5316
local.bibliographicCitation.startpage5307
local.contributor.affiliationDevlin, Jennifer, Peter MacCallum Cancer Centre
local.contributor.affiliationHannan, Katherine, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationNg, Pui Y., Peter MacCallum Cancer Centre
local.contributor.affiliationBywater, Megan J., Peter MacCallum Cancer Centre
local.contributor.affiliationShortt, Jake, Peter MacCallum Cancer Centre
local.contributor.affiliationCullinane, C, Peter MacCallum Cancer Centre
local.contributor.affiliationMcArthur, Grant, Peter MacCallum Cancer Centre
local.contributor.affiliationJohnstone, Ricky, Peter MacCallum Cancer Centre
local.contributor.affiliationHannan, Ross, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationPearson, Richard B, Peter MacCallum Cancer Centre
local.contributor.authoruidHannan, Katherine, u1000189
local.contributor.authoruidHannan, Ross, u1000203
local.description.embargo2037-12-31
local.description.notesImported from ARIES
local.identifier.absfor111201 - Cancer Cell Biology
local.identifier.absfor111206 - Haematological Tumours
local.identifier.absfor111207 - Molecular Targets
local.identifier.ariespublicationa383154xPUB1123
local.identifier.citationvolume280
local.identifier.doi10.1111/febs.12135
local.identifier.scopusID2-s2.0-84886095337
local.type.statusPublished Version

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