Please use this identifier to cite or link to this item: https://doi.org/10.7554/ELIFE.61287
Title: Characterization of the mechanism by which the rb/e2f pathway controls expression of the cancer genomic dna deaminase apobec3b
Authors: Roelofs, P.A.
Goh, C.Y. 
Chua, B.H. 
Jarvis, M.C.
Stewart, T.A.
McCann, J.L.
McDougle, R.M.
Carpenter, M.A.
Martens, J.W.M.
Span, P.N.
Kappei, D. 
Harris, R.S.
Keywords: APOBEC3B
Cancer mutagenesis
Cell cycle regulation
DREAM complex
Polyomavirus T antigen
PRC1.6 complex
RB/E2F pathway
Transcriptional regulation
Issue Date: 2020
Publisher: eLife Sciences Publications Ltd
Citation: Roelofs, P.A., Goh, C.Y., Chua, B.H., Jarvis, M.C., Stewart, T.A., McCann, J.L., McDougle, R.M., Carpenter, M.A., Martens, J.W.M., Span, P.N., Kappei, D., Harris, R.S. (2020). Characterization of the mechanism by which the rb/e2f pathway controls expression of the cancer genomic dna deaminase apobec3b. eLife 9 : 1-64. ScholarBank@NUS Repository. https://doi.org/10.7554/ELIFE.61287
Abstract: APOBEC3B (A3B)-catalyzed DNA cytosine deamination contributes to the overall mutational landscape in breast cancer. Molecular mechanisms responsible for A3B upregulation in cancer are poorly understood. Here, we show that a single E2F cis-element mediates repression in normal cells and that expression is activated by its mutational disruption in a reporter construct or the endogenous A3B gene. The same E2F site is required for A3B induction by polyomavirus T antigen indicating a shared molecular mechanism. Proteomic and biochemical experiments demonstrate binding of wildtype but not mutant E2F promoters by repressive PRC1.6/E2F6 and DREAM/E2F4 complexes. Knockdown and overexpression studies confirm involvement of these repressive complexes in regulating A3B expression. Altogether, these studies demonstrate that A3B expression is suppressed in normal cells by repressive E2F complexes and that viral or mutational disruption of this regulatory network triggers overexpression in breast cancer and provides fuel for tumor evolution. © 2020, eLife Sciences Publications Ltd. All rights reserved.
Source Title: eLife
URI: https://scholarbank.nus.edu.sg/handle/10635/197512
ISSN: 2050084X
DOI: 10.7554/ELIFE.61287
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