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免疫球蛋白μ重链基因增强子B细胞特异性结构域上的一种三蛋白-DNA复合物。

A three-protein-DNA complex on a B cell-specific domain of the immunoglobulin mu heavy chain gene enhancer.

作者信息

Rao E, Dang W, Tian G, Sen R

机构信息

Rosenstiel Basic Medical Sciences Research Center and Departments of Biology, Brandeis University, Waltham, Massachusetts 02254-9110, USA.

出版信息

J Biol Chem. 1997 Mar 7;272(10):6722-32. doi: 10.1074/jbc.272.10.6722.

Abstract

The lymphoid-specific immunoglobulin mu heavy chain gene intron enhancer (muE) contains multiple binding sites for trans-acting nuclear factors. We have used a combination of in vitro and in vivo assays to reconstruct protein-DNA interactions on a minimal B cell-specific mu enhancer that contains three motifs, muA, muB, and muE3. Using ETS-domain proteins that transactivate the minimal enhancer in non-lymphoid cells, we show that (i) PU.1 binds coordinately to both muA and muB sites in vitro and (ii) in the presence of Ets-1, this factor binds to the muA site and PU.1 to the muB site. Two factors, TFE3 and USF, bind to the muE3 element. When the ETS proteins are present together with muE3 binding proteins, a three-protein-DNA complex is generated. Furthermore, we provide evidence for protein-protein interactions between Ets-1 and PU.1 proteins that bind to muA and muB sites, and between Ets-1 and TFE3 bound to the muA and mu3 sites. We propose that this domain of the mu enhancer is assembled into a nucleoprotein complex that contains two tissue-restricted ETS domain proteins that recognize DNA from the same side of the helix and one ubiquitously expressed bHLH-leucine zipper protein that binds between them, recognizing its site from a different side of the helix.

摘要

淋巴细胞特异性免疫球蛋白μ重链基因内含子增强子(μE)含有多个反式作用核因子的结合位点。我们利用体外和体内试验相结合的方法,在一个包含三个基序(μA、μB和μE3)的最小B细胞特异性μ增强子上重建蛋白质-DNA相互作用。使用能在非淋巴细胞中反式激活最小增强子的ETS结构域蛋白,我们发现:(i)PU.1在体外能协同结合μA和μB位点;(ii)在Ets-1存在的情况下,该因子结合μA位点,而PU.1结合μB位点。两个因子,TFE3和USF,结合到μE3元件上。当ETS蛋白与μE3结合蛋白同时存在时,会形成一个三蛋白-DNA复合物。此外,我们提供了证据,证明结合在μA和μB位点上的Ets-1与PU.1蛋白之间,以及结合在μA和μ3位点上的Ets-1与TFE3之间存在蛋白质-蛋白质相互作用。我们提出,μ增强子的这个结构域被组装成一个核蛋白复合物,该复合物包含两个组织限制性的ETS结构域蛋白,它们从螺旋的同一侧识别DNA,以及一个普遍表达的bHLH-亮氨酸拉链蛋白,该蛋白结合在它们之间,从螺旋的另一侧识别其位点。

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