Disparate ligand-mediated Ca(2+) responses by wild-type, mutant Ser(200)Ala and Ser(204)Ala alpha(2A)-adrenoceptor: G(alpha15) fusion proteins: evidence for multiple ligand-activation binding sites.

PauwelsPJ; ColpaertFC

首页> 外文期刊>British Journal of Pharmacology >Disparate ligand-mediated Ca(2+) responses by wild-type, mutant Ser(200)Ala and Ser(204)Ala alpha(2A)-adrenoceptor: G(alpha15) fusion proteins: evidence for multiple ligand-activation binding sites.

【24h】

Disparate ligand-mediated Ca(2+) responses by wild-type, mutant Ser(200)Ala and Ser(204)Ala alpha(2A)-adrenoceptor: G(alpha15) fusion proteins: evidence for multiple ligand-activation binding sites.

机译：野生型，突变体Ser（200）Ala和Ser（204）Ala alpha（2A）-肾上腺素受体：G（alpha15）融合蛋白的不同的配体介导的Ca（2+）反应：多个配体激活结合位点的证据。

获取原文

获取原文并翻译 | 示例

获取外文期刊封面封底 >>

开具论文收录证明 >>

文献代查 >>

页面导航

摘要
著录项
相似文献
相关主题

摘要

Ligand : receptor interactions were analysed at wt, mutant Ser(200)Ala and Ser(204)Ala alpha(2A) ARs by measuring Ca(2+) responses in CHO-K1 cells either by co-expression with a G(alpha15) protein or at a receptor : G(alpha15) protein stoichiometry of 1.0 using fusion proteins. The magnitude of the UK 14304-mediated Ca(2+) response as elicited by a G(alpha15) protein was largest with both mutant Ser(200)Ala and Ser(204)Ala alpha(2A)ARs compared to the wt alpha(2A) AR in the co-expression and fusion protein experiments. The activation profiles of the wt and both mutant alpha(2A) ARs as analysed by a series of alpha(2) AR agonists differed. d-Medetomidine and clonidine appeared most efficacious at the Ser(204)Ala alpha(2A) AR, whereas oxymetazoline was also partially active at the Ser(200)Ala alpha(2A) AR. Talipexole was silent at both mutant alpha(2A) ARs. The intrinsic activity of (-)-adrenaline was either absent or partial at the Ser(204)Ala and Ser(200)Ala alpha(2A) AR, respectively. This latter observation is related to its lower binding affinity for both mutant alpha(2A) ARs. Ligands characterized as antagonists at wt and Ser(200)Ala alpha(2A) ARs demonstrated either no intrinsic activity (i.e., RX 811059) or positive efficacy with a different rank order of maximal response at the Ser(204)Ala alpha(2A) AR (atipamezole=SKF 86466=idazoxan>dexefaroxan) than Asp(79)Asn alpha(2A) AR (atipamezole>idazoxan approximately SKF 86466>dexefaroxan) and Thr(373)Lys alpha(2A) AR (SKF 86466>atipamezole approximately idazoxan>dexefaroxan). These effects were only observed in the co-expression experiments at concentrations in line with their binding affinities. In conclusion, these Ca(2+) data suggest that multiple activation binding sites exist for these ligands at the alpha(2A) AR, and that their activation may be affected in different ways by the mutations being investigated.

机译：配体：受体相互作用进行了分析wt，突变体Ser（200）Ala和Ser（204）Ala alpha（2A）ARs，通过测量CHO-K1细胞中的Ca（2+）反应，或者与G（alpha15）共表达蛋白或受体：使用融合蛋白的G（alpha15）蛋白化学计量为1.0。由G（alpha15）蛋白质引起的UK 14304介导的Ca（2+）反应的幅度最大，突变型Ser（200）Ala和Ser（204）Ala alpha（2A）ARs与wt alpha（ 2A）AR在共表达和融合蛋白实验中的作用。 wt和两个突变体alpha（2A）ARs的激活曲线（通过一系列alpha（2）AR激动剂分析）不同。 d-美托咪定和可乐定似乎在Ser（204）Ala alpha（2A）AR上最有效，而羟甲唑啉在Ser（200）Ala alpha（2A）AR上也部分起作用。 Talipexole在两个突变体alpha（2A）AR沉默。（-）-肾上腺素的固有活性分别在Ser（204）Ala和Ser（200）Ala alpha（2A）AR处不存在或不存在。后者的观察结果与其对两个突变体alpha（2A）AR的较低结合亲和力有关。在wt和Ser（200）Ala alpha（2A）AR处表现为拮抗剂的配体表现出无内在活性（即RX 811059）或阳性功效，并且在Ser（204）Ala alpha（2A）处具有最大反应的不同等级AR（atipamezole = SKF 86466 = idazoxan> dexefaroxan）比Asp（79）Asn alpha（2A）AR（atipamezole> idazoxan约为SKF 86466> dexefaroxan）和Thr（373）Lys alpha（2A）AR（SKF 86466> atipamezole约为idazoxan > dexfaroxan）。仅在共表达实验中以与其结合亲和力一致的浓度观察到了这些作用。总之，这些Ca（2+）数据表明在alpha（2A）AR处存在这些配体的多个激活结合位点，并且它们的激活可能受到所研究突变的影响而有所不同。

著录项

来源
《British Journal of Pharmacology》 |2000年第7期|P.1505-1512|共8页
作者
PauwelsPJ; ColpaertFC;
展开▼
作者单位

Department of Cellular and Molecular Biology, Centre de Recherche Pierre Fabre, 17, avenue Jean Moulin 81106 Castres Cedex, France. peter.pauwels;

ierre-fabre.com;

展开▼
收录信息美国《科学引文索引》(SCI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
原文格式 PDF
正文语种 eng
中图分类药理学;
关键词
Calcium; Heterotrimeric GTP Binding Proteins metabolism; Receptors; Adrenergic; alpha-2; 钙; 受体; 肾上腺素能α2;

机译：Calcium;Heterotrimeric GTP Binding Proteins metabolism;Receptors;Adrenergic;alpha-2;钙;受体;肾上腺素能α2;

相似文献

外文文献

1. Agonist efficacy at the alpha2A-adrenoceptor:G alpha15 fusion protein: an analysis based on Ca2+ responses. [J] . Pauwels PJ, Finana F, Tardif S, Naunyn-Schmiedeberg's Archives of Pharmacology . 2000,第6期

机译：在alpha2A-肾上腺素受体：G alpha15融合蛋白上的激动剂功效：基于Ca2 +响应的分析。
2. Ligand-receptor interactions as controlled by wild-type and mutant Thr(370)Lys alpha2B-adrenoceptor-Galpha15 fusion proteins. [J] . Pauwels PJ, Tardif S, Finana F, Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry . 2000,第1期

机译：受野生型和突变型Thr（370）Lys alpha2B-肾上腺素受体-Galpha15融合蛋白控制的配体-受体相互作用。
3. A novel mutant 10Ala/Arg together with mutant 144Ser/Arg of hepatitis B virus X protein involved in hepatitis B virus-related hepatocarcinogenesis in HepG2 cell lines [J] . Shi Ying, Wang Junwei, Wang Yuhe, Cancer letters . 2016,第2期

机译：涉及乙肝病毒相关肝癌发生的乙肝病毒X蛋白的新型突变体10Ala / Arg和突变体144Ser / Arg
4. Disparate ligand-mediated Ca2+ responses by wild-type mutant Ser200Ala and Ser204Ala α2A-adrenoceptor : Gα15 fusion proteins: evidence for multiple ligand-activation binding sites [O] . P J Pauwels, F C Colpaert 2000

机译：野生型突变体Ser200Ala和Ser204Alaα2A-肾上腺素受体：Gα15融合蛋白对配体介导的Ca2 +响应的不同：多个配体激活结合位点的证据
5. Disparate ligand-mediated Ca2+ responses by wild-type, mutant Ser200Ala and Ser204Ala α2A-adrenoceptor : Gα15 fusion proteins: evidence for multiple ligand-activation binding sites [O] . Pauwels, P J, Colpaert, F C 2000

机译：野生型突变体Ser200Ala和Ser204Alaα2A-肾上腺素受体：Gα15融合蛋白对配体介导的Ca2 +响应的不同：多个配体激活结合位点的证据

Disparate ligand-mediated Ca(2+) responses by wild-type, mutant Ser(200)Ala and Ser(204)Ala alpha(2A)-adrenoceptor: G(alpha15) fusion proteins: evidence for multiple ligand-activation binding sites.

摘要

著录项

相似文献

相关主题

期刊订阅