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Biochemical analyses of the AF10 protein: the extended LAP/PHD-finger mediates oligomerisation.

Linder, B; Newman, R; Jones, L K; Debernardi, S; Young, B D; Freemont, P; Verrijzer, C P; Saha, V

J Mol Biol. 2000;299(2):369-78.

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Abstract

Leukaemogenesis correlates with alterations in chromatin structure brought about by the gain or loss of interactive domains from regulatory factors that are disrupted by chromosomal translocations. The gene MLL, a target of such translocation events, forms chimaeric fusion products with a variety of partner genes. While MLL appears to be involved in chromatin-mediated gene regulation, the functions of its partner genes are largely speculative. We report the biochemical analysis of the MLL partner gene AF10 and its possible role in leukaemogenesis. AF10 has been reported to be re-arranged with genes other than MLL leading to the same phenotype, a myeloid leukaemia. We have identified a novel protein-protein interaction motif in the AF10 protein comprising the extended LAP/PHD-finger. This domain mediates homo-oligomerisation of recombinant AF10 and is conserved in several proteins, including MLL itself. AF10 binds cruciform DNA via a specific interaction with an AT-hook motif and is localised to the nucleus by a defined bipartite nuclear localisation signal in the N-terminal region.

Bibliographic metadata

Type of resource:
Content type:
Published date:
Abbreviated journal title:
ISSN:
Place of publication:
ENGLAND
Volume:
299
Issue:
2
Pagination:
369-78
Digital Object Identifier:
10.1006/jmbi.2000.3766
Pubmed Identifier:
10860745
Pii Identifier:
S0022-2836(00)93766-5
Access state:
Active

Institutional metadata

University researcher(s):

Record metadata

Manchester eScholar ID:
uk-ac-man-scw:85943
Created by:
Saha, Vaskar
Created:
6th July, 2010, 15:10:53
Last modified by:
Saha, Vaskar
Last modified:
6th July, 2010, 15:10:53

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