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果蝇的esc和E(z)蛋白是多梳蛋白介导的基因沉默中的直接伙伴。

The Drosophila esc and E(z) proteins are direct partners in polycomb group-mediated repression.

作者信息

Jones C A, Ng J, Peterson A J, Morgan K, Simon J, Jones R S

机构信息

Department of Biological Sciences, Southern Methodist University, Dallas, Texas 75275-0376, USA.

出版信息

Mol Cell Biol. 1998 May;18(5):2825-34. doi: 10.1128/MCB.18.5.2825.

Abstract

The extra sex combs (esc) and Enhancer of zeste [E(z)] proteins are members of the Drosophila Polycomb group (Pc-G) of transcriptional repressors. Here we present evidence for direct physical interaction between the esc and E(z) proteins using yeast two-hybrid and in vitro binding assays. In addition, coimmunoprecipitation from embryo extracts demonstrates association of esc and E(z) in vivo. We have delimited the esc-binding domain of E(z) to an N-terminal 33-amino-acid region. Furthermore, we demonstrate that site-directed mutations in the esc protein previously shown to impair esc function in vivo disrupt esc-E(z) interactions in vitro. We also show an in vitro interaction between the heed and EZH1 proteins, which are human homologs of esc and E(z), respectively. These results suggest that the esc-E(z) molecular partnership has been conserved in evolution. Previous studies suggested that esc is primarily involved in the early stages of Pc-G-mediated silencing during embryogenesis. However, E(z) is continuously required in order to maintain chromosome binding by other Pc-G proteins. In light of these earlier observations and the molecular data presented here, we discuss how esc-E(z) protein complexes may contribute to transcriptional silencing by the Pc-G.

摘要

额外性梳(esc)蛋白和zeste增强子[E(z)]蛋白是果蝇转录抑制因子多梳家族(Pc-G)的成员。在此,我们通过酵母双杂交和体外结合试验,提供了esc蛋白和E(z)蛋白之间直接物理相互作用的证据。此外,从胚胎提取物中进行的共免疫沉淀证明了esc和E(z)在体内的关联。我们已将E(z)的esc结合结构域限定为N端的一个33个氨基酸的区域。此外,我们证明,先前显示在体内损害esc功能的esc蛋白中的定点突变,在体外破坏了esc-E(z)相互作用。我们还展示了heed蛋白和EZH1蛋白之间的体外相互作用,它们分别是esc和E(z)的人类同源物。这些结果表明,esc-E(z)分子伙伴关系在进化过程中得到了保守。先前的研究表明,esc主要参与胚胎发育过程中Pc-G介导的沉默的早期阶段。然而,为了维持其他Pc-G蛋白与染色体的结合,持续需要E(z)。鉴于这些早期观察结果和此处呈现的分子数据,我们讨论了esc-E(z)蛋白复合物可能如何通过Pc-G促成转录沉默。

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