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ETO, but not leukemogenic fusion protein AML1/ETO, augments RBP-Jkappa/SHARP-mediated repression of Notch target genes

ETO, but not leukemogenic fusion protein AML1/ETO, augments RBP-Jkappa/SHARP-mediated repression of Notch target genes
ETO, but not leukemogenic fusion protein AML1/ETO, augments RBP-Jkappa/SHARP-mediated repression of Notch target genes
Notch is a transmembrane receptor that determines cell fates and pattern formation in all animal species. After specific ligand binding, the intracellular part of Notch is cleaved off and translocates to the nucleus, where it targets the DNA binding protein RBP-J. In the absence of Notch, RBP-J represses Notch target genes by recruiting a corepressor complex. We and others have previously identified SHARP as one component of this complex. Here, we show that the corepressor ETO as well as the leukemogenic fusion protein AML1/ETO directly interacts with SHARP, that ETO is part of the endogenous RBP-J-containing corepressor complex, and that ETO is found at Notch target gene promoters. In functional assays, corepressor ETO, but not AML1/ETO, augments SHARP-mediated repression in an histone deacetylase-dependent manner. Furthermore, either the knockdown of ETO or the overexpression of AML1/ETO activates Notch target genes. Therefore, we propose that AML1/ETO can disturb the normal, repressive function of ETO at Notch target genes. This activating (or derepressing) effect of AML1/ETO may contribute to its oncogenic potential in myeloid leukemia.
0270-7306
3502-3512
Salat, D.
ec4e36dc-cfff-4ff3-ab84-f8a87b43a7f9
Liefke, R.
ab36b0f7-0640-405a-9577-7d33ad7d68ac
Wiedenmann, J.
ad445af2-680f-4927-90b3-589ac9d538f7
Borggrefe, T.
599d1b4a-2d5e-422b-8d02-2d76e37c49a9
Oswald, F.
8fea64d4-21b7-4f41-93dd-0c4ce331c84b
Salat, D.
ec4e36dc-cfff-4ff3-ab84-f8a87b43a7f9
Liefke, R.
ab36b0f7-0640-405a-9577-7d33ad7d68ac
Wiedenmann, J.
ad445af2-680f-4927-90b3-589ac9d538f7
Borggrefe, T.
599d1b4a-2d5e-422b-8d02-2d76e37c49a9
Oswald, F.
8fea64d4-21b7-4f41-93dd-0c4ce331c84b

Salat, D., Liefke, R., Wiedenmann, J., Borggrefe, T. and Oswald, F. (2008) ETO, but not leukemogenic fusion protein AML1/ETO, augments RBP-Jkappa/SHARP-mediated repression of Notch target genes. Molecular and Cellular Biology, 28 (10), 3502-3512. (doi:10.1128/MCB.01966-07).

Record type: Article

Abstract

Notch is a transmembrane receptor that determines cell fates and pattern formation in all animal species. After specific ligand binding, the intracellular part of Notch is cleaved off and translocates to the nucleus, where it targets the DNA binding protein RBP-J. In the absence of Notch, RBP-J represses Notch target genes by recruiting a corepressor complex. We and others have previously identified SHARP as one component of this complex. Here, we show that the corepressor ETO as well as the leukemogenic fusion protein AML1/ETO directly interacts with SHARP, that ETO is part of the endogenous RBP-J-containing corepressor complex, and that ETO is found at Notch target gene promoters. In functional assays, corepressor ETO, but not AML1/ETO, augments SHARP-mediated repression in an histone deacetylase-dependent manner. Furthermore, either the knockdown of ETO or the overexpression of AML1/ETO activates Notch target genes. Therefore, we propose that AML1/ETO can disturb the normal, repressive function of ETO at Notch target genes. This activating (or derepressing) effect of AML1/ETO may contribute to its oncogenic potential in myeloid leukemia.

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Published date: May 2008

Identifiers

Local EPrints ID: 51155
URI: http://eprints.soton.ac.uk/id/eprint/51155
ISSN: 0270-7306
PURE UUID: 5787456f-733a-4d4c-8098-3e035b8f6d44
ORCID for J. Wiedenmann: ORCID iD orcid.org/0000-0003-2128-2943

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Date deposited: 07 May 2008
Last modified: 16 Mar 2024 03:53

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Contributors

Author: D. Salat
Author: R. Liefke
Author: J. Wiedenmann ORCID iD
Author: T. Borggrefe
Author: F. Oswald

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