Characterization of the DOT1L Network: Implications of Diverse Roles for DOT1L

被引:0
|
作者
Geunyeong Park
Zihua Gong
Junjie Chen
Ja-Eun Kim
机构
[1] Kyung Hee University,Department of Pharmacology, School of Medicine
[2] The University of Texas M.D. Anderson Cancer Center,Department of Experimental Radiation Oncology
来源
The Protein Journal | 2010年 / 29卷
关键词
Affinity purification; AF9; DOT1L; ENL; NPM1;
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暂无
中图分类号
学科分类号
摘要
Methylation of lysine 79 on histone H3 (H3K79) is mediated by a methyltransferase called Dot1-like protein (DOT1L). DOT1L is involved in the regulation of telomeric silencing, development, cell cycle checkpoint and transcription. However, the mechanisms by which DOT1L controls these unrelated and diverse functions are unknown. To gain greater insight into DOT1L-mediated functions, we have purified a DOT1L-containing complex using tandem affinity purification. Mass spectrometry of the DOT1L-containing complex revealed that AF9, ENL and NPM1 were shown to be major DOT1L-interacting proteins. To construct a plausible DOT1L-interaction web, AF9-, ENL- and NPM1-containing complexes were also purified for mass spectrometry analysis. The data showed that DOT1L might control AF9- and ENL-mediated transcription, regulate RNA processing, and function as a histone chaperone in a NPM1-dependent manner. In addition, the purification of protein complexes identified a number of novel interacting partners associated with DOT1L, AF9, ENL and NPM1. These data define a unique DOT1L network and shed light on unknown functions of the DOT1L complex.
引用
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页码:213 / 223
页数:10
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