Two distinct nuclear receptor interaction domains in NSD1, a novel SET protein that exhibits characteristics of both corepressors and coactivators

被引:210
作者
Huang, NW [1 ]
vom Baur, E [1 ]
Garnier, JM [1 ]
Lerouge, T [1 ]
Vonesch, JL [1 ]
Lutz, Y [1 ]
Chambon, P [1 ]
Losson, R [1 ]
机构
[1] Coll France, ULP, INSERM, CNRS,Inst Genet & Biol Mol & Cellulaire, F-67404 Illkirch Graffenstaden, Strasbourg, France
关键词
activation function AF-2; chromatin; PHD finger; SET domain; transcriptional intermediary factor;
D O I
10.1093/emboj/17.12.3398
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
NSD1, a novel 2588 amino acid mouse nuclear protein that interacts directly with the ligand-binding domain (LBD) of several nuclear receptors (NRs), has been identified and characterized. NSD1 contains a SET domain and multiple PHD fingers. In addition to these conserved domains found in both positive and negative Drosophila chromosomal regulators, NSD1 contains two distinct NR interaction domains, NID-L and NID+L that exhibit binding properties of NIDs found in NR corepressors and coactivators, respectively. NID-L, but not NID+L, interacts with the unliganded LBDs of retinoic acid receptors (RAR) and thyroid hormone receptors (TR), and this interaction is severely impaired by mutations in the LED alpha-helix 1 that prevent binding of corepressors and transcriptional silencing by apo-NRs, NID+L, but not NID-L, interacts with the liganded LBDs of RAR, TR, retinoid X receptor (RXR), and estrogen receptor (ER), and this interaction is abrogated by mutations in the LED alpha-helix 1 that prevent binding of coactivators of the ligand-induced transcriptional activation function AF-2, A novel variant (FxxLL) of the NR box motif (LxxLL) is present in NID+L and is required for the binding of NSD1 to holo-LBDs. Interestingly, NSD1 contains separate repression and activation domains. Thus, NSD1 may define a novel class of bifunctional transcriptional intermediary factors playing distinct roles in both the presence and absence of ligand.
引用
收藏
页码:3398 / 3412
页数:15
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