Evolutionary selection across the nuclear hormone receptor superfamily with a focus on the NR1I subfamily (vitamin D, pregnane X, and constitutive androstane receptors).

Matthew D Krasowski, Kazuto Yasuda, Lee R Hagey, Erin G Schuetz
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引用次数: 77

Abstract

Background: The nuclear hormone receptor (NR) superfamily complement in humans is composed of 48 genes with diverse roles in metabolic homeostasis, development, and detoxification. In general, NRs are strongly conserved between vertebrate species, and few examples of molecular adaptation (positive selection) within this superfamily have been demonstrated. Previous studies utilizing two-species comparisons reveal strong purifying (negative) selection of most NR genes, with two possible exceptions being the ligand-binding domains (LBDs) of the pregnane X receptor (PXR, NR1I2) and the constitutive androstane receptor (CAR, NR1I3), two proteins involved in the regulation of toxic compound metabolism and elimination. The aim of this study was to apply detailed phylogenetic analysis using maximum likelihood methods to the entire complement of genes in the vertebrate NR superfamily. Analyses were carried out both across all vertebrates and limited to mammals and also separately for the two major domains of NRs, the DNA-binding domain (DBD) and LBD, in addition to the full-length sequences. Additional functional data is also reported for activation of PXR and the vitamin D receptor (VDR; NR1I1) to gain further insight into the evolution of the NR1I subfamily.

Results: The NR genes appear to be subject to strong purifying selection, particularly in the DBDs. Estimates of the ratio of the non-synonymous to synonymous nucleotide substitution rates (the omega ratio) revealed that only the PXR LBD had a sub-population of codons with an estimated omega ratio greater than 1. CAR was also unusual in showing high relative omega ratios in both the DBD and LBD, a finding that may relate to the recent appearance of the CAR gene (presumably by duplication of a pre-mammalian PXR gene) just prior to the evolution of mammals. Functional analyses of the NR1I subfamily show that human and zebrafish PXRs show similar activation by steroid hormones and early bile salts, properties not shared by sea lamprey, mouse, or human VDRs, or by Xenopus laevis PXRs.

Conclusion: NR genes generally show strong sequence conservation and little evidence for positive selection. The main exceptions are PXR and CAR, genes that may have adapted to cross-species differences in toxic compound exposure.

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核激素受体超家族的进化选择,重点是NR1I亚家族(维生素D,孕激素X和构成雄烷受体)。
背景:人类核激素受体(NR)超家族补体由48个基因组成,在代谢稳态、发育和解毒等方面发挥着不同的作用。一般来说,NRs在脊椎动物物种之间是高度保守的,在这个超家族中很少有分子适应(正选择)的例子被证明。先前利用两种比较的研究表明,大多数NR基因具有强的纯化(负)选择,但两个可能的例外是妊娠X受体(PXR, NR1I2)和构成型雄甾受体(CAR, NR1I3)的配体结合域(lbd),这两个蛋白质参与有毒化合物代谢和消除的调节。本研究的目的是利用最大似然方法对脊椎动物NR超家族的全部基因进行详细的系统发育分析。除了全长序列外,还对所有脊椎动物和哺乳动物进行了分析,并分别对NRs的两个主要结构域,dna结合结构域(DBD)和LBD进行了分析。还报道了PXR和维生素D受体(VDR)激活的其他功能数据;以进一步了解NR1I亚家族的进化。结果:NR基因似乎受到强烈的纯化选择,特别是在dbd中。对非同义核苷酸取代率与同义核苷酸取代率之比(omega比率)的估计显示,只有PXR LBD具有估计omega比率大于1的密码子亚群。CAR在DBD和LBD中也显示出较高的相对omega比率,这一发现可能与CAR基因在哺乳动物进化之前的最近出现(可能是通过复制前哺乳动物PXR基因)有关。NR1I亚家族的功能分析表明,人类和斑马鱼的PXRs在类固醇激素和早期胆汁盐的作用下表现出相似的激活,这是海七鳃鳗、小鼠、人类vdr或非洲爪蟾PXRs所不具有的特性。结论:NR基因普遍具有较强的序列保守性,正选择证据较少。主要的例外是PXR和CAR基因,它们可能已经适应了有毒化合物暴露的跨物种差异。
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