Biology Department, Kenyon College , Gambier, Ohio 43022, United States.
Biochemistry. 2013 Mar 12;52(10):1746-54. doi: 10.1021/bi301722k. Epub 2013 Feb 27.
The aryl hydrocarbon receptor (AHR) is a Per-ARNT-Sim (PAS) family protein that mediates the toxicity of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) in vertebrates. Frogs are remarkably insensitive to TCDD, and AHRs from Xenopus laevis bind TCDD with low affinity. We sought to identify structural features of X. laevis AHR1β associated with low TCDD sensitivity. Substitution of the entire ligand binding domain (LBD) with the corresponding sequence from mouse AHR(b-1) dramatically increased TCDD responsiveness in transactivation assays. To identify the amino acid residues responsible, we constructed a comparative model of the AHR1β LBD using homologous domains of PAS proteins HIF2α and ARNT. The model revealed an internal cavity with dimensions similar to those of the putative binding cavity of mouse AHR(b-1), suggesting the importance of side chain interactions over cavity size. Of residues with side chains clearly pointing into the cavity, only two differed from the mouse sequence. When A354, located within a conserved β-strand, was changed to serine, the corresponding mouse residue, the EC50 for TCDD decreased more than 15-fold. When N325 was changed to serine, the EC50 decreased 3-fold. When the mutations were combined, the EC50 decreased from 18.6 to 0.8 nM, the value nearly matching the TCDD sensitivity of mouse AHR. Velocity sedimentation analysis confirmed that mutant frog AHRs exhibited correspondingly increased levels of TCDD binding. We also assayed mutant AHRs for responsiveness to a candidate endogenous ligand, 6-formylindolo[3,2-b]carbazole (FICZ). Mutations that increased sensitivity to TCDD also increased sensitivity to FICZ. This comparative study represents a novel approach to discerning fundamental information about the structure of AHR and its interactions with biologically important agonists.
芳香烃受体(AHR)是一个 PER-ARNT-SIM(PAS)家族蛋白,在脊椎动物中介导 2,3,7,8-四氯二苯并-p-二恶英(TCDD)的毒性。青蛙对 TCDD 表现出惊人的不敏感性,并且来自非洲爪蟾的 AHR 与 TCDD 的结合亲和力低。我们试图确定与低 TCDD 敏感性相关的非洲爪蟾 AHR1β 的结构特征。用来自小鼠 AHR(b-1)的相应序列替代整个配体结合域(LBD),在反式激活测定中极大地增加了 TCDD 的反应性。为了确定负责的氨基酸残基,我们使用 PAS 蛋白 HIF2α 和 ARNT 的同源结构域构建了 AHR1β LBD 的比较模型。该模型显示了一个具有与假定的小鼠 AHR(b-1)结合腔相似尺寸的内部腔,表明侧链相互作用的重要性超过腔的大小。在明显指向腔的侧链的残基中,只有两个与小鼠序列不同。当位于保守β-链内的 A354 残基被改变为丝氨酸时,对应的小鼠残基,TCDD 的 EC50 降低了 15 倍以上。当 N325 被改变为丝氨酸时,EC50 降低了 3 倍。当突变组合时,EC50 从 18.6 降低到 0.8 nM,接近小鼠 AHR 的 TCDD 敏感性。速度沉降分析证实突变的青蛙 AHR 表现出相应增加的 TCDD 结合水平。我们还检测了突变的 AHR 对候选内源性配体 6-甲酰基吲哚并[3,2-b]咔唑(FICZ)的反应性。增加对 TCDD 的敏感性的突变也增加了对 FICZ 的敏感性。这项比较研究代表了一种新的方法,可以深入了解 AHR 的结构及其与生物重要激动剂的相互作用的基本信息。