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作为诱导型增强子的雌激素反应元件:DNA序列要求及向糖皮质激素反应元件的转化

The estrogen-responsive element as an inducible enhancer: DNA sequence requirements and conversion to a glucocorticoid-responsive element.

作者信息

Martinez E, Givel F, Wahli W

机构信息

Institut de Biologie Animale, Université de Lausanne, Switzerland.

出版信息

EMBO J. 1987 Dec 1;6(12):3719-27. doi: 10.1002/j.1460-2075.1987.tb02706.x.

Abstract

The estrogen-responsive element (ERE) present in the 5'-flanking region of the Xenopus laevis vitellogenin (vit) gene B1 has been characterized by transient expression analysis of chimeric vit-tk-CAT (chloramphenicol acetyltransferase) gene constructs transfected into the human estrogen-responsive MCF-7 cell line. The vit B1 ERE behaves like an inducible enhancer, since it is able to confer estrogen inducibility to the heterologous HSV thymidine kinase (tk) promoter in a relative position- and orientation-independent manner. In this assay, the minimal B1 ERE is 33 bp long and consists of two 13 bp imperfect palindromic elements both of which are required for the enhancer activity. A third imperfect palindromic element is present further upstream within the 5'-flanking region of the gene but is unable to confer hormone responsiveness by itself. Similarly, neither element forming the B1 ERE can alone confer estrogen inducibility to the tk promoter. However, in combinations of two, all three imperfect palindromes can act cooperatively to form a functional ERE. In contrast a single 13 bp perfect palindromic element, GGTCACTGTGACC, such as the one found upstream of the vit gene A2, is itself sufficient to act as a fully active ERE. Single point mutations within this element abolish estrogen inducibility, while a defined combination of two mutations converts this ERE into a glucocorticoid-responsive element.

摘要

非洲爪蟾卵黄蛋白原(vit)基因B1的5'侧翼区域存在的雌激素反应元件(ERE),已通过对转染到人雌激素反应性MCF-7细胞系中的嵌合vit-tk-CAT(氯霉素乙酰转移酶)基因构建体进行瞬时表达分析来进行表征。vit B1 ERE的行为类似于可诱导增强子,因为它能够以相对位置和方向独立的方式赋予异源单纯疱疹病毒胸苷激酶(tk)启动子雌激素诱导性。在该分析中,最小的B1 ERE长33 bp,由两个13 bp的不完全回文元件组成,这两个元件对于增强子活性都是必需的。在该基因的5'侧翼区域的更上游还存在第三个不完全回文元件,但它自身不能赋予激素反应性。同样,形成B1 ERE的任何一个元件都不能单独赋予tk启动子雌激素诱导性。然而,两个元件组合时,所有三个不完全回文序列可以协同作用形成一个功能性ERE。相比之下,一个单一的13 bp完美回文元件GGTCACTGTGACC,例如在vit基因A2上游发现的那个元件,其本身就足以作为一个完全活性的ERE发挥作用。该元件内的单点突变会消除雌激素诱导性,而两个突变的特定组合会将这个ERE转化为糖皮质激素反应元件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/62eb/553842/0b925ad43881/emboj00252-0160-a.jpg

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