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果蝇蜕皮激素受体的A、B1和B2亚型对基因活性的差异调控。

Differential control of gene activity by isoforms A, B1 and B2 of the Drosophila ecdysone receptor.

作者信息

Mouillet J F, Henrich V C, Lezzi M, Vögtli M

机构信息

Institute for Cell Biology, ETH-Hönggerberg, Zürich, Switzerland.

出版信息

Eur J Biochem. 2001 Mar;268(6):1811-9.

PMID:11248701
Abstract

The steroid hormone ecdysone initiates molting and metamorphosis in Drosophila via a heterodimeric receptor consisting of EcR that binds hormone, and USP, a homolog of the vertebrate RXR receptor. EcR exists in three isoforms EcRA, EcRB1 and EcRB2 that are thought to direct specific physiological responses to ecdysone. These three isoforms differ only in their N-terminal A/B domain that implies that sequences responsible for the differential physiological effects lie within the A/B domains of the EcR isoforms. In the present study, we set out to determine the capability of the three isoforms and their A/B domains to control gene transcription. When full-length EcR plasmids were cotransfected into mammalian cells with a USP expressing and a cognate reporter plasmid, the three EcR isoforms showed striking differences in their ability to control gene transcription, both in the presence and in the absence of hormone. Furthermore, the A/B domains of EcRB1 and of EcRB2 when fused to the GAL4 DNA binding domain are sufficient to activate transcription of a reporter gene, in yeast as well as in mammalian cells. In contrast, a fusion construct containing the A/B domain of EcRA represses basal transcription of the reporter gene. All these findings emphasize the importance of the A/B domains of the three EcR isoforms for differentially controlling gene transcription. Furthermore, they provide evidence for the existence of an autonomous ligand-independent activation function (AF1) in the A/B domains of EcRB1 and EcRB2 and of an inhibitory function (IF) in the A/B domain of EcRA.

摘要

类固醇激素蜕皮激素通过一种异源二聚体受体在果蝇中启动蜕皮和变态过程,该受体由结合激素的EcR和脊椎动物RXR受体的同源物USP组成。EcR存在三种异构体EcRA、EcRB1和EcRB2,它们被认为介导对蜕皮激素的特定生理反应。这三种异构体仅在其N端A/B结构域有所不同,这表明负责差异生理效应的序列位于EcR异构体的A/B结构域内。在本研究中,我们着手确定这三种异构体及其A/B结构域控制基因转录的能力。当将全长EcR质粒与表达USP的质粒和同源报告质粒共转染到哺乳动物细胞中时,无论有无激素,三种EcR异构体在控制基因转录的能力上都表现出显著差异。此外,EcRB1和EcRB2的A/B结构域与GAL4 DNA结合结构域融合后,在酵母和哺乳动物细胞中均足以激活报告基因的转录。相比之下,含有EcRA的A/B结构域的融合构建体则抑制报告基因的基础转录。所有这些发现都强调了三种EcR异构体的A/B结构域对差异控制基因转录的重要性。此外,它们还为EcRB1和EcRB2的A/B结构域中存在自主的非配体依赖性激活功能(AF1)以及EcRA的A/B结构域中存在抑制功能(IF)提供了证据。

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