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光滑双脐螺视黄酸X受体激动剂结合配体结合结构域新型四聚体复合物的晶体结构

Crystal structure of a novel tetrameric complex of agonist-bound ligand-binding domain of Biomphalaria glabrata retinoid X receptor.

作者信息

de Groot Arjan, de Rosny Eve, Juillan-Binard Céline, Ferrer Jean-Luc, Laudet Vincent, Pierce Raymond J, Pebay-Peyroula Eva, Fontecilla-Camps Juan Carlos, Borel Franck

机构信息

Laboratoire de Cristallographie et Cristallogenèse des Protéines, Institut de Biologie Structurale 'Jean-Pierre Ebel' (UMR 5075, CEA-CNRS-UJF), 41 rue Jules Horowitz, 38027 Grenoble cedex 1, France.

出版信息

J Mol Biol. 2005 Dec 9;354(4):841-53. doi: 10.1016/j.jmb.2005.09.090. Epub 2005 Oct 21.

DOI:10.1016/j.jmb.2005.09.090
PMID:16274693
Abstract

Nuclear receptors form an important class of transcription regulators in metazoans. To learn more about the evolution of these proteins, we have initiated structural studies on nuclear receptor ligand-binding domains from various animals. Here we present the crystal structure of the ligand-binding domain (LBD) of the retinoid X receptor (RXR) from the mollusc Biomphalaria glabrata. The structure reveals a novel tetrameric association in which each monomer is complexed to the human RXR ligand 9-cis retinoic acid and to a human co-activator-derived peptide. The ligand and the co-activator peptide are bound in essentially the same manner as observed in previously reported human RXR LBD structures, suggesting that the mechanisms of RXR-mediated transcription regulation are very similar in mollusc and human. The structure shows further that binding of ligand and co-activator peptide does not necessarily lead to the typical holo-conformation in which helix 12 (H12) folds back and packs against the LBD. Within a canonical dimer, only one monomer is in this closed agonist conformation. The other monomer is in an open conformation with H12 protruding from the LBD core, occupying the H12 interaction groove of another open monomer in an adjacent dimer in a domain swapping fashion, thus resulting in a tetrameric association. Additional tetramer interfaces are formed between H11 of the closed LBD and H6 of the open LBD. This novel holo-tetramer configuration may have a biological role in activating genes whose promoters are poorly recognised by dimers but much more efficiently by the corresponding tetramers.

摘要

核受体是后生动物中一类重要的转录调节因子。为了更深入了解这些蛋白质的进化过程,我们开展了对来自不同动物的核受体配体结合结构域的结构研究。在此,我们展示了来自软体动物光滑双脐螺的类视黄醇X受体(RXR)配体结合结构域(LBD)的晶体结构。该结构揭示了一种新型的四聚体缔合,其中每个单体都与人类RXR配体9-顺式视黄酸以及一个源自人类共激活因子的肽形成复合物。配体和共激活因子肽的结合方式与先前报道的人类RXR LBD结构基本相同,这表明在软体动物和人类中,RXR介导的转录调节机制非常相似。该结构还进一步表明,配体和共激活因子肽的结合不一定会导致典型的全构象,即螺旋12(H12)向后折叠并与LBD堆积。在一个典型的二聚体中,只有一个单体处于这种封闭的激动剂构象。另一个单体处于开放构象,H12从LBD核心突出,以结构域交换的方式占据相邻二聚体中另一个开放单体的H12相互作用凹槽,从而形成四聚体缔合。在封闭LBD的H11和开放LBD的H6之间形成了额外的四聚体界面。这种新型的全四聚体构型可能在激活那些启动子难以被二聚体识别但能被相应四聚体更高效识别的基因方面具有生物学作用。

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