假定的褪黑素受体拮抗剂GR128107对非洲爪蟾黑素细胞是一种部分激动剂。

The putative melatonin receptor antagonist GR128107 is a partial agonist on Xenopus laevis melanophores.

作者信息

Teh M T, Sugden D

机构信息

Biomedical Sciences Division, King's College London.

出版信息

Br J Pharmacol. 1999 Mar;126(5):1237-45. doi: 10.1038/sj.bjp.0702404.

DOI:10.1038/sj.bjp.0702404

PMID:10205014

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1565880/

Abstract

GR128107 (3-(1-acetyl-3-methyl-piperidine)-5-methoxyindole) has previously been reported to be a competitive melatonin receptor antagonist in blocking melatonin inhibition of [3H]-dopamine release from rabbit retina, a response mediated by the MT2 receptor subtype. 2. GR128107, like melatonin, induced a rapid (maximum response in 60-90 min) pigment aggregation in a clonal line of Xenopus laevis melanophores. GR128107 behaved as a partial agonist (pEC50 8.58+/-0.03, n=3) with an Emax of 0.83 (relative to melatonin, pEC50 10.09+/-0.03, n=3). 3. The concentration-response curve for pigment granule aggregation to both melatonin and GR128107 was displaced in a parallel, rightward manner by melatonin receptor antagonists with very similar potencies; estimated pKB RJ252 (against melatonin 4.60/against GR128107 4.54) < GR135533 (6.40/6.14) < Luzindole (6.45/6.49) < S20929 (6.58/6.65) < 4-P-PDOT (6.73/6.85). 4. Both melatonin- and GR128107-induced pigment granule aggregation was prevented by pretreatment of melanophores with pertussis toxin (10-1000 ng ml(-1)). 5. Prolonged pre-treatment of melanophores with melatonin desensitized the pigment aggregation response to GR128107. In desensitized cells, the maximal aggregation produced by GR128107 was only 0.27+/-0.01 (n=4) and the pEC50 was reduced (vehicle 8.57+/-0.12; melatonin pre-treated 7.84+/-0.09, n=4). The maximal response to melatonin in desensitized melanophores was unchanged but the pEC50 was reduced (vehicle 10.49+/-0.03; melatonin pre-treated 9.83+/-0.04, n=4). 6. These results demonstrate that GR128107 induces pigment granule aggregation in Xenopus melanophores by activating a cell membrane melatonin receptor coupled via a pertussis toxin-sensitive G-protein. 7. The partial agonist activity of GR128107 in melanophores may be apparent because of the very high density of melatonin receptors in these cells (Bmax 1223 fmol mg protein(-1)) compared to the low density of sites in rabbit retina (Bmax 3.1 fmol mg protein(-1)). This suggestion is supported by the finding that GR128107, like melatonin, acted as a full agonist and inhibited forskolin-stimulation of cyclic AMP accumulation in NIH-3T3 cells expressing a high density of human mt1 or MT2 receptors.

摘要

GR128107（3-(1-乙酰基-3-甲基-哌啶)-5-甲氧基吲哚）先前已有报道，它在阻断褪黑素对兔视网膜[3H]-多巴胺释放的抑制作用方面是一种竞争性褪黑素受体拮抗剂，该反应由MT2受体亚型介导。2. GR128107与褪黑素一样，在非洲爪蟾黑素细胞的克隆系中诱导了快速的（60 - 90分钟达到最大反应）色素聚集。GR128107表现为部分激动剂（pEC50 8.58±0.03，n = 3），Emax为0.83（相对于褪黑素，pEC50 10.09±0.03，n = 3）。3. 褪黑素受体拮抗剂以平行、右移的方式使色素颗粒聚集对褪黑素和GR128107的浓度 - 反应曲线发生位移，其效力非常相似；估计的pKB值RJ252（对褪黑素4.60/对GR128107 4.54）< GR135533（6.40/6.14）< 鲁辛朵（6.45/6.49）< S20929（6.58/6.65）< 4-P-PDOT（6.73/6.85）。4. 用百日咳毒素（10 - 1000 ng ml(-1)）预处理黑素细胞可阻止褪黑素和GR128107诱导的色素颗粒聚集。5. 用褪黑素对黑素细胞进行长时间预处理会使对GR128107的色素聚集反应脱敏。在脱敏细胞中，GR128107产生的最大聚集仅为0.27±0.01（n = 4），pEC50降低（溶剂对照8.57±0.12；褪黑素预处理7.84±0.09，n = 4）。脱敏黑素细胞对褪黑素的最大反应未改变，但pEC50降低（溶剂对照10.49±0.03；褪黑素预处理9.83±0.04，n = 4）。6. 这些结果表明，GR128107通过激活经由百日咳毒素敏感的G蛋白偶联的细胞膜褪黑素受体，在非洲爪蟾黑素细胞中诱导色素颗粒聚集。7. GR128107在黑素细胞中的部分激动剂活性可能很明显，因为与兔视网膜中低密度的位点（Bmax 3.1 fmol mg蛋白(-1)）相比，这些细胞中褪黑素受体的密度非常高（Bmax 1223 fmol mg蛋白(-1)）。这一推测得到以下发现的支持：GR128107与褪黑素一样，在表达高密度人mt1或MT2受体的NIH - 3T3细胞中作为完全激动剂起作用，并抑制福斯可林对环磷酸腺苷积累的刺激。