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Structure of the histone chaperone CIA/ASF1--double bromodomain complex linking histone modifications and site-specific histone eviction

Authors :
Akai, Yusuke
Adachi, Naruhiko
Hayashi, Yohei
Eitoku, Masamitsu
Sano, Norihiko
Natsume, Ryo
Kudo, Norio
Tanokura, Masaru
Senda, Toshiya
Horikoshi, Masami
Source :
Proceedings of the National Academy of Sciences of the United States. May 4, 2010, Vol. 107 Issue 18, p8153, 6 p.
Publication Year :
2010

Abstract

Nucleosomes around the promoter region are disassembled for transcription in response to various signals, such as acetylation and methylation of histones. Although the interactions between histone-acetylation-recognizing bromodomains and factors involved in nucleosome disassembly have been reported, no structural basis connecting histone modifications and nucleosome disassembly has been obtained. Here, we determined at 3.3 [Angstrom] resolution the crystal structure of histone chaperone cell cycle gene 1 (CCG1) interacting factor A/antisilencing function 1 (CIA/ASF1) in complex with the double bromodomain in the CCG1/TAF1/TAF(II)250 subunit of transcription factor lID. Structural, biochemical, and biological studies suggested that interaction between double bromodomain and CIA/ASF1 is required for their colocalization, histone eviction, and pol II entry at active promoter regions. Furthermore, the present crystal structure has characteristics that can connect histone acetylation and CIA/ASFl-mediated histone eviction. These findings suggest that the molecular complex between CIA/ASF1 and the double bromodomain plays a key role in site-specific histone eviction at active promoter regions. The model we propose here is the initial structure-based model of the biological signaling from histone modifications to structural change of the nucleosome (hi-MOST model). chromatin | transcription | transcription factor IID | x-ray crystallography doi/10.1073/pnas.0912509107

Details

Language :
English
ISSN :
00278424
Volume :
107
Issue :
18
Database :
Gale General OneFile
Journal :
Proceedings of the National Academy of Sciences of the United States
Publication Type :
Academic Journal
Accession number :
edsgcl.226632692