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章鱼雌激素受体与雌二醇的三维模型分析:阻碍雌激素结合的空间冲突证据。

Analysis of 3D models of octopus estrogen receptor with estradiol: evidence for steric clashes that prevent estrogen binding.

作者信息

Baker Michael E, Chandsawangbhuwana Charlie

机构信息

Department of Medicine, University of California, San Diego, 9500 Gilman Drive, La Jolla, CA 92093-0693, USA.

出版信息

Biochem Biophys Res Commun. 2007 Sep 28;361(3):782-8. doi: 10.1016/j.bbrc.2007.07.110. Epub 2007 Jul 30.

Abstract

Relatives of the vertebrate estrogen receptor (ER) are found in Aplysia californica, Octopus vulgaris, Thais clavigera, and Marisa cornuarietis. Unlike vertebrate ERs, invertebrate ERs are constitutively active and do not bind estradiol. To investigate the molecular basis of the absence of estrogen binding, we constructed a 3D model of the putative steroid-binding domain on octopus ER. Our 3D model indicates that binding of estradiol to octopus ER is prevented by steric clashes between estradiol and amino acids in the steroid-binding pocket. In this respect, octopus ER resembles vertebrate estrogen-related receptors (ERR), which have a ligand-binding pocket that cannot accommodate estradiol. Like ERR, octopus ER also may have the activation function 2 domain (AF2) in a configuration that can bind to coactivators in the absence of estrogens, which would explain constitutive activity of octopus ER.

摘要

在加州海兔、普通章鱼、疣荔枝螺和大瓶螺中发现了脊椎动物雌激素受体(ER)的亲属。与脊椎动物的ER不同,无脊椎动物的ER具有组成型活性,且不与雌二醇结合。为了研究缺乏雌激素结合的分子基础,我们构建了章鱼ER上假定的类固醇结合结构域的三维模型。我们的三维模型表明,雌二醇与章鱼ER的结合受到雌二醇与类固醇结合口袋中的氨基酸之间空间冲突的阻碍。在这方面,章鱼ER类似于脊椎动物雌激素相关受体(ERR),后者具有一个无法容纳雌二醇的配体结合口袋。与ERR一样,章鱼ER也可能具有激活功能2结构域(AF2),其构型能够在没有雌激素的情况下与共激活因子结合,这可以解释章鱼ER的组成型活性。

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