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Structure-based analysis of the ultraspiracle protein and docking studies of putative ligands

机译:基于超结构蛋白的结构分析和推定配体的对接研究

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摘要

The ultraspiracle protein (USP) is the insect ortholog of the mammalian retinoid X receptor (RXR). Fundamental questions concern the functional role of USP as the heterodimerization partner of insect nuclear receptors such as the ecdysone receptor. The crystallographic structures of the ligand binding domain of USPs of Heliothis virescens and Drosophila melanogaster solved recently show that helix 12 is locked in an antagonist conformation raising the question whether USPs could adopt an agonist conformation as observed in RXRα. In order to investigate this hypothesis, a homology model for USP is proposed that allows a structural analysis of the agonist conformation of helix 12 based on the sequence comparison with RXR. For USP, one of the main issues concerns its function and in particular whether its activity is ligand independent or not. The x-ray structures strongly suggest that USP can bind ligands. Putative ligands have therefore been docked in the USP homology model. Juvenile hormones and juvenile hormone analogs were chosen as target ligands for the docking study. The interaction between the ligand and the receptor are examined in terms of the pocket shape as well as in terms of the chemical nature of the residues lining the ligand binding cavity.
机译:超细气管蛋白(USP)是哺乳动物类维生素A X受体(RXR)的昆虫直系同源物。基本问题涉及USP作为昆虫核受体(如蜕皮激素受体)的异源二聚体伴侣的功能。最近解毒的Heliothis virescens和果蝇Drosophila melanogaster的USP的配体结合结构域的晶体结构显示,螺旋12被锁定在拮抗剂构象中,这引发了一个问题,即USP是否可以采用在RXRα中观察到的激动剂构象。为了研究该假设,提出了USP的同源性模型,其允许基于与RXR的序列比较对螺旋12的激动剂构象进行结构分析。对于USP,主要问题之一是其功能,尤其是其活性是否与配体无关。 X射线结构强烈暗示USP可以结合配体。因此,推定的配体已停靠在USP同源性模型中。选择少年激素和少年激素类似物作为对接研究的靶配体。根据口袋形状以及衬在配体结合腔中的残基的化学性质来检查配体与受体之间的相互作用。

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