Human HDAC1 and HDAC2 function in the DNA-damage response to promote DNA nonhomologous end-joining

被引:493
|
作者
Miller, Kyle M. [1 ]
Tjeertes, Jorrit V. [1 ]
Coates, Julia [1 ]
Legube, Gaelle [2 ,3 ]
Polo, Sophie E. [1 ]
Britton, Sebastien [1 ]
Jackson, Stephen P. [1 ]
机构
[1] Univ Cambridge, Gurdon Inst, Cambridge, England
[2] Univ Toulouse, Toulouse, France
[3] Ctr Natl Rech Sci, Lab Biol Cellulaire & Mol Controle Proliferat, Toulouse, France
来源
NATURE STRUCTURAL & MOLECULAR BIOLOGY | 2010年 / 17卷 / 09期
基金
英国生物技术与生命科学研究理事会; 英国惠康基金;
关键词
DOUBLE-STRAND BREAKS; HISTONE DEACETYLASE INHIBITORS; ACETYLATION; REPAIR; CHECKPOINT; SENESCENCE; CHROMATIN; H3; GAMMA-H2AX; P53;
D O I
10.1038/nsmb.1899
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
DNA double-strand break (DSB) repair occurs within chromatin and can be modulated by chromatin-modifying enzymes. Here we identify the related human histone deacetylases HDAC1 and HDAC2 as two participants in the DNA-damage response. We show that acetylation of histone H3 Lys56 (H3K56) was regulated by HDAC1 and HDAC2 and that HDAC1 and HDAC2 were rapidly recruited to DNA-damage sites to promote hypoacetylation of H3K56. Furthermore, HDAC1- and 2-depleted cells were hypersensitive to DNA-damaging agents and showed sustained DNA-damage signaling, phenotypes that reflect defective DSB repair, particularly by nonhomologous end-joining (NHEJ). Collectively, these results show that HDAC1 and HDAC2 function in the DNA-damage response by promoting DSB repair and thus provide important insights into the radio-sensitizing effects of HDAC inhibitors that are being developed as cancer therapies.
引用
收藏
页码:1144 / U15
页数:9
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