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蜕皮激素受体复合物在核心识别基序处的高水平反式激活。

High level transactivation by the ecdysone receptor complex at the core recognition motif.

作者信息

Vögtli M, Elke C, Imhof M O, Lezzi M

机构信息

Institute for Cell Biology, ETH-Hönggerberg, CH-8093 Zürich, Switzerland.

出版信息

Nucleic Acids Res. 1998 May 15;26(10):2407-14. doi: 10.1093/nar/26.10.2407.

Abstract

Ecdysteroid signaling in insects is mediated by the ecdysone receptor complex that is composed of a heterodimer of the ecdysone receptor and Ultraspiracle. The DNA binding specificity plays a critical role of defining the repertoire of target genes that respond to the hormone. We report here the determination of the preferred core recognition motif by a binding site selection procedure. The consensus sequence consists of a perfect palindrome of the heptameric half-site sequence GAGGTCA that is separated by a single A/T base pair. No binding polarity of the ecdysone receptor/Ultraspiracle heterodimer to the core recognition motif was observed. This core motif mediated the highest level of ligand-induced transactivation when compared to a series of synthetic ecdysone response elements and to the natural element of the Drosophila hsp27 gene. This is the first report of a palindromic sequence identified as the highest affinity DNA binding site for a heterodimeric nuclear hormone receptor complex. We further present evidence that the ligand of the ecdysone receptor preferentially drives Ultraspiracle from a homodimer into a heterodimer. This mechanism might contribute additionally to a tight control of target gene expression.

摘要

昆虫中的蜕皮甾类信号传导由蜕皮激素受体复合物介导,该复合物由蜕皮激素受体和超气门蛋白的异二聚体组成。DNA结合特异性在定义响应激素的靶基因库中起着关键作用。我们在此报告通过结合位点选择程序确定的首选核心识别基序。共有序列由七聚体半位点序列GAGGTCA的完美回文组成,中间由单个A/T碱基对隔开。未观察到蜕皮激素受体/超气门蛋白异二聚体对核心识别基序的结合极性。与一系列合成蜕皮激素反应元件以及果蝇hsp27基因的天然元件相比,该核心基序介导了最高水平的配体诱导的反式激活。这是首次报道将回文序列鉴定为异二聚体核激素受体复合物的最高亲和力DNA结合位点。我们进一步提供证据表明,蜕皮激素受体的配体优先将超气门蛋白从同二聚体驱动为异二聚体。这种机制可能还有助于对靶基因表达进行严格控制。

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