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对来自无脊椎脊索动物文昌鱼的非重复视黄酸X核受体配体结合域的结构和功能见解。

Structural and functional insights into the ligand-binding domain of a nonduplicated retinoid X nuclear receptor from the invertebrate chordate amphioxus.

作者信息

Tocchini-Valentini Giuseppe D, Rochel Natacha, Escriva Hector, Germain Pierre, Peluso-Iltis Carole, Paris Mathilde, Sanglier-Cianferani Sarah, Van Dorsselaer Alain, Moras Dino, Laudet Vincent

机构信息

Département de Biologie et de Génomique Structurales and Département Biologie du Cancer, Institut de Génétique et de Biologie Moléculaire et Cellulaire, UMR7104 CNRS, U596 INSERM, Université Louis Pasteur, 67400 Illkirch, France.

出版信息

J Biol Chem. 2009 Jan 16;284(3):1938-48. doi: 10.1074/jbc.M805692200. Epub 2008 Nov 4.

DOI:10.1074/jbc.M805692200
PMID:18986992
Abstract

Retinoid X nuclear receptors (RXRs), as well as their insect orthologue, ultraspiracle protein (USP), play an important role in the transcription regulation mediated by the nuclear receptors as the common partner of many other nuclear receptors. Phylogenetic and structural studies have shown that the several evolutionary shifts have modified the ligand binding ability of RXRs. To understand the vertebrate-specific character of RXRs, we have studied the RXR ligand-binding domain of the cephalochordate amphioxus (Branchiostoma floridae), an invertebrate chordate that predates the genome duplication that produced the three vertebrates RXRs (alpha, beta, and gamma). Here we report the crystal structure of a novel apotetramer conformation of the AmphiRXR ligand-binding domain, which shows some similarity with the structures of the arthropods RXR/USPs. AmphiRXR adopts an apo antagonist conformation with a peculiar conformation of helix H11 filling the binding pocket. In contrast to the arthropods RXR/USPs, which cannot be activated by any RXR ligands, our functional data show that AmphiRXR, like the vertebrates/mollusk RXRs, is able to bind and be activated by RXR ligands but less efficiently than vertebrate RXRs. Our data suggest that amphioxus RXR is, functionally, an intermediate between arthropods RXR/USPs and vertebrate RXRs.

摘要

维甲酸X核受体(RXRs)及其昆虫同源物超气门蛋白(USP),作为许多其他核受体的共同伙伴,在核受体介导的转录调控中发挥着重要作用。系统发育和结构研究表明,几次进化转变改变了RXRs的配体结合能力。为了了解RXRs的脊椎动物特异性特征,我们研究了头索动物文昌鱼(佛罗里达文昌鱼)的RXR配体结合结构域,文昌鱼是一种无脊椎动物,在产生三种脊椎动物RXRs(α、β和γ)的基因组复制之前就已存在。在此,我们报道了AmphiRXR配体结合结构域一种新的无配体四聚体构象的晶体结构,该结构与节肢动物RXR/USPs的结构有一些相似之处。AmphiRXR采用无配体拮抗剂构象,螺旋H11具有独特构象填充结合口袋。与不能被任何RXR配体激活的节肢动物RXR/USPs不同,我们的功能数据表明,AmphiRXR与脊椎动物/软体动物RXRs一样,能够结合RXR配体并被其激活,但效率低于脊椎动物RXRs。我们的数据表明,文昌鱼RXR在功能上是节肢动物RXR/USPs和脊椎动物RXRs之间的中间体。

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Structural and functional insights into the ligand-binding domain of a nonduplicated retinoid X nuclear receptor from the invertebrate chordate amphioxus.对来自无脊椎脊索动物文昌鱼的非重复视黄酸X核受体配体结合域的结构和功能见解。
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