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Mxi1是一种与Max特异性相互作用以结合Myc-Max识别位点的蛋白质。

Mxi1, a protein that specifically interacts with Max to bind Myc-Max recognition sites.

作者信息

Zervos A S, Gyuris J, Brent R

机构信息

Department of Genetics, Harvard Medical School, Boston, Massachusetts 02114.

出版信息

Cell. 1993 Jan 29;72(2):223-32. doi: 10.1016/0092-8674(93)90662-a.

Abstract

We used the interaction trap to isolate a novel human protein that specifically interacts with Max. This protein, Mxi1 (for Max interactor 1), contains a bHLH-Zip motif that is similar to that found in Myc family proteins. Mxi1 interacts specifically with Max to form heterodimers that efficiently bind to the Myc-Max consensus recognition site. When bound to DNA by a LexA moiety in yeast, Mxi1 does not stimulate transcription. mxi1 mRNA is expressed in many tissues, and its expression is elevated in U-937 myeloid leukemia cells that have been stimulated to differentiate. These facts are consistent with a model in which Mxi1-Max heterodimers indirectly inhibit Myc function in two ways: first, by sequestering Max, thus preventing the formation of Myc-Max heterodimers, and second, by competing with Myc-Max heterodimers for binding to target sites.

摘要

我们利用相互作用陷阱分离出一种与Max特异性相互作用的新型人类蛋白质。这种蛋白质,即Mxi1(Max相互作用蛋白1),含有一个bHLH-Zip基序,与Myc家族蛋白质中的基序相似。Mxi1与Max特异性相互作用形成异源二聚体,该异源二聚体可有效结合到Myc-Max共有识别位点。当通过酵母中的LexA部分与DNA结合时,Mxi1不会刺激转录。mxi1 mRNA在许多组织中表达,并且在已被刺激分化的U-937髓样白血病细胞中其表达升高。这些事实与一个模型一致,在该模型中,Mxi1-Max异源二聚体通过两种方式间接抑制Myc功能:第一,通过隔离Max,从而阻止Myc-Max异源二聚体的形成;第二,通过与Myc-Max异源二聚体竞争结合靶位点。

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