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CP2与GATA-1在红细胞启动子调控中的功能相互作用。

Functional interaction of CP2 with GATA-1 in the regulation of erythroid promoters.

作者信息

Bosè Francesca, Fugazza Cristina, Casalgrandi Maura, Capelli Alessia, Cunningham John M, Zhao Quan, Jane Stephen M, Ottolenghi Sergio, Ronchi Antonella

机构信息

Dipartimento di Biotecnologie e Bioscienze, Università di Milano-Bicocca, P.za della Scienza 2, 20126 Milano, Italy.

出版信息

Mol Cell Biol. 2006 May;26(10):3942-54. doi: 10.1128/MCB.26.10.3942-3954.2006.

Abstract

We observed that binding sites for the ubiquitously expressed transcription factor CP2 were present in regulatory regions of multiple erythroid genes. In these regions, the CP2 binding site was adjacent to a site for the erythroid factor GATA-1. Using three such regulatory regions (from genes encoding the transcription factors GATA-1, EKLF, and p45 NF-E2), we demonstrated the functional importance of the adjacent CP2/GATA-1 sites. In particular, CP2 binds to the GATA-1 HS2 enhancer, generating a ternary complex with GATA-1 and DNA. Mutations in the CP2 consensus greatly impaired HS2 activity in transient transfection assays with K562 cells. Similar results were obtained by transfection of EKLF and p45 NF-E2 mutant constructs. Chromatin immunoprecipitation with K562 cells showed that CP2 binds in vivo to all three regulatory elements and that both GATA-1 and CP2 were present on the same GATA-1 and EKLF regulatory elements. Adjacent CP2/GATA-1 sites may represent a novel module for erythroid expression of a number of genes. Additionally, coimmunoprecipitation and glutathione S-transferase pull-down experiments demonstrated a physical interaction between GATA-1 and CP2. This may contribute to the functional cooperation between these factors and provide an explanation for the important role of ubiquitous CP2 in the regulation of erythroid genes.

摘要

我们观察到,普遍表达的转录因子CP2的结合位点存在于多个红系基因的调控区域。在这些区域,CP2结合位点与红系因子GATA-1的位点相邻。利用三个这样的调控区域(来自编码转录因子GATA-1、EKLF和p45 NF-E2的基因),我们证明了相邻的CP2/GATA-1位点的功能重要性。特别是,CP2与GATA-1 HS2增强子结合,与GATA-1和DNA形成三元复合物。在K562细胞的瞬时转染实验中,CP2共有序列中的突变极大地损害了HS2活性。通过转染EKLF和p45 NF-E2突变构建体也获得了类似结果。用K562细胞进行的染色质免疫沉淀显示,CP2在体内与所有三个调控元件结合,并且GATA-1和CP2都存在于相同的GATA-1和EKLF调控元件上。相邻的CP2/GATA-1位点可能代表了许多基因红系表达的一个新模块。此外,免疫共沉淀和谷胱甘肽S-转移酶下拉实验证明了GATA-1和CP2之间存在物理相互作用。这可能有助于这些因子之间的功能协作,并为普遍存在的CP2在红系基因调控中的重要作用提供一个解释。

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