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人类内皮素受体的不同亚结构域决定了它们对内皮素A选择性拮抗剂和内皮素B选择性激动剂的选择性。

Distinct subdomains of human endothelin receptors determine their selectivity to endothelinA-selective antagonist and endothelinB-selective agonists.

作者信息

Sakamoto A, Yanagisawa M, Sawamura T, Enoki T, Ohtani T, Sakurai T, Nakao K, Toyo-oka T, Masaki T

机构信息

Department of Pharmacology, Faculty of Medicine, Kyoto University, Japan.

出版信息

J Biol Chem. 1993 Apr 25;268(12):8547-53.

PMID:8473300
Abstract

The endothelin (ET) family of peptides acts via two subtypes of G-protein-coupled heptahelical receptors termed ETA and ETB, which have distinct rank orders of affinity to endothelin receptor agonists and antagonists. To delineate which portions of the receptor molecules determine ligand selectivity, we have constructed a series of chimeras between human ETA and ETB receptors and characterized the chimeric receptors expressed in heterologous cell lines by competitive radioligand binding analysis and by measuring agonist-induced transients of intracellular Ca2+. We demonstrate that the binding determinant for the ETB-selective agonists ET-3, BQ3020, and IRL1620 residues within the region spanning the putative transmembrane helices IV-VI and the adjacent loop regions. In contrast, the transmembrane helices I, II, III, and VII plus the intervening loop regions specify the selectivity for BQ123, an ETA-selective antagonist. BQ123 exhibited no detectable agonistic activity in all wild-type and chimeric receptors tested. A chimeric receptor that has the transmembrane helices IV-VI (and adjacent loops) from the ETB receptor inserted into the remaining regions from the ETA receptor binds both the ETA- and ETB-selective ligands with high affinities. Moreover, BQ123 competitively inhibits the binding of the amino-terminally truncated ETB agonists, 125I-BQ3020 and 125I-IRL1620, to this chimeric receptor, suggesting that BQ123 is a mimic of the carboxyl-terminal linear portion of endothelins. These findings indicate that there are at least two separable ligand interaction subdomains within the endothelin receptors.

摘要

内皮素(ET)肽家族通过两种G蛋白偶联的七螺旋受体亚型(称为ETA和ETB)发挥作用,这两种受体对内皮素受体激动剂和拮抗剂具有不同的亲和力排序。为了确定受体分子的哪些部分决定配体选择性,我们构建了一系列人ETA和ETB受体之间的嵌合体,并通过竞争性放射性配体结合分析以及测量激动剂诱导的细胞内Ca2+瞬变来表征在异源细胞系中表达的嵌合受体。我们证明,ETB选择性激动剂ET-3、BQ3020和IRL1620的结合决定簇位于跨越假定跨膜螺旋IV-VI及相邻环区的区域内。相比之下,跨膜螺旋I、II、III和VII加上中间的环区决定了ETA选择性拮抗剂BQ123的选择性。BQ123在所有测试的野生型和嵌合受体中均未表现出可检测到的激动活性。一种将ETB受体的跨膜螺旋IV-VI(及相邻环)插入ETA受体其余区域的嵌合受体,对ETA和ETB选择性配体均具有高亲和力结合。此外,BQ123竞争性抑制氨基末端截短的ETB激动剂125I-BQ3020和125I-IRL1620与该嵌合受体的结合,表明BQ123是内皮素羧基末端线性部分的模拟物。这些发现表明内皮素受体中至少存在两个可分离的配体相互作用亚结构域。

相似文献

1
Distinct subdomains of human endothelin receptors determine their selectivity to endothelinA-selective antagonist and endothelinB-selective agonists.人类内皮素受体的不同亚结构域决定了它们对内皮素A选择性拮抗剂和内皮素B选择性激动剂的选择性。
J Biol Chem. 1993 Apr 25;268(12):8547-53.
2
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The ligand-receptor interactions of the endothelin systems are mediated by distinct "message" and "address" domains.内皮素系统的配体-受体相互作用由不同的“信息”和“地址”结构域介导。
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Novel ligands BQ123 and BQ3020 characterize endothelin receptor subtypes ETA and ETB in human kidney.新型配体BQ123和BQ3020可区分人肾中的内皮素受体亚型ETA和ETB。
Kidney Int. 1993 Jul;44(1):36-42. doi: 10.1038/ki.1993.210.
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ETA and ETB endothelin receptors in human myometrium characterized by the subtype selective ligands BQ123, BQ3020, FR139317 and PD151242.人子宫肌层中的ETA和ETB内皮素受体通过亚型选择性配体BQ123、BQ3020、FR139317和PD151242进行表征。
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Characterization of [125I]-endothelin-1 and [125I]-BQ3020 binding to rat cerebellar endothelin receptors.[125I] -内皮素-1和[125I] -BQ3020与大鼠小脑内皮素受体结合的特性研究
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Characterization of the endothelin receptor selective agonist, BQ3020 and antagonists BQ123, FR139317, BQ788, 50235, Ro462005 and bosentan in the heart.内皮素受体选择性激动剂BQ3020以及拮抗剂BQ123、FR139317、BQ788、50235、Ro462005和波生坦在心脏中的特性研究
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Mol Pharmacol. 1997 Oct;52(4):582-9. doi: 10.1124/mol.52.4.582.
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Pseudo-noncompetitive antagonism by BQ123 of intracellular calcium transients mediated by human ETA endothelin receptor.BQ123对人ETA内皮素受体介导的细胞内钙瞬变的拟非竞争性拮抗作用。
Biochem Biophys Res Commun. 1994 Apr 29;200(2):679-86. doi: 10.1006/bbrc.1994.1504.
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Characterization of three non-peptide endothelin receptor ligands using human cloned ETA and ETB receptors.利用人克隆的ETA和ETB受体对三种非肽类内皮素受体配体进行表征。
Br J Pharmacol. 1994 Aug;112(4):1251-7. doi: 10.1111/j.1476-5381.1994.tb13218.x.

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