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生长抑素与L-362855对人重组sst4受体的差异激动剂活性

Differential agonist activity of somatostatin and L-362855 at human recombinant sst4 receptors.

作者信息

Smalley K S, Feniuk W, Humphrey P P

机构信息

Glaxo Institute of Applied Pharmacology, Department of Pharmacology, University of Cambridge.

出版信息

Br J Pharmacol. 1998 Oct;125(4):833-41. doi: 10.1038/sj.bjp.0702133.

DOI:10.1038/sj.bjp.0702133
PMID:9831922
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1571016/
Abstract
  1. The operational characteristics of somatostatin (SRIF) sst4 receptors are poorly understood. In this study, we have characterized human recombinant sst4 receptors expressed in CHO cells (CHOsst4) by radioligand binding and microphysiometry. 2. Increasing concentrations SRIF or other SRIF receptor ligands inhibited specific [125I]-Tyr11-SRIF binding in CHOsst4 cell membranes with respective pIC50 values of SRIF (8.82), L-362855 (7.40), BIM-23027 (<5.5) and MK-678 (<5.5). 3. These ligands displayed agonist activity, producing concentration-dependent increases in rates of extracellular acidification (EAR) with pEC50 values of SRIF (9.6) and L-362855 (8.0), respectively. BIM-23027 and MK-678 were at least 1000 times weaker than SRIF. The SRIF maximum was about 40% of that observed with L-362855. 4. In the presence of SRIF (0.1-1 nM), concentration-effect curves to L-362855 were displaced to the right with a progressive reduction in the L-362855 maximum. 5. When cells were only exposed to a single maximally effective concentration of SRIF or L-362855, there was no difference in the magnitude of the agonist-induced increase in EAR. However, a second agonist challenge, 30 min later showed that responses to SRIF but not L-362855 were markedly desensitized. 6. When concentration-effect curves to SRIF and L-362855 were obtained by combining data from cells exposed to only a single agonist concentration, SRIF (pEC50 9.2) was approximately 20 times more potent than L-362855 (pEC50 8.0) but the maxima were the same. Responses to both SRIF and L-362855 were abolished by pertussis toxin. 7. SRIF and L-362855-induced increases in EAR were inhibited by N-ethyl isopropyl amiloride (10 microM) but were not modified by inhibitors of PKC (Go-6976), MAP kinase (PD-98059), tyrosine kinase (genistein) or tyrosine phosphatase (sodium orthovanadate). 8. The results suggest that SRIF-induced increases in EAR in CHOsst4 cells involved activation of the Na+/H+ antiporter and were mediated via Gi/Go G proteins. Responses to SRIF, but not L-362855, were subject to marked desensitization which may be a consequence of differential activation of receptor-effector coupling pathways.
摘要
  1. 生长抑素(SRIF)sst4受体的操作特性了解甚少。在本研究中,我们通过放射性配体结合和微生理测定法对在CHO细胞(CHOsst4)中表达的人重组sst4受体进行了表征。2. 增加SRIF或其他SRIF受体配体的浓度可抑制CHOsst4细胞膜中特异性[125I]-Tyr11-SRIF结合,SRIF、L-362855、BIM-23027和MK-678的各自pIC50值分别为8.82、7.40、<5.5和<5.5。3. 这些配体表现出激动剂活性,使细胞外酸化速率(EAR)呈浓度依赖性增加,SRIF和L-362855的pEC50值分别为9.6和8.0。BIM-23027和MK-678的活性比SRIF至少弱1000倍。SRIF的最大效应约为L-362855所观察到的最大效应的40%。4. 在存在SRIF(0.1 - 1 nM)的情况下,L-362855的浓度 - 效应曲线向右移动,L-362855的最大效应逐渐降低。5. 当细胞仅暴露于单一最大有效浓度的SRIF或L-362855时,激动剂诱导的EAR增加幅度没有差异。然而,30分钟后第二次激动剂刺激表明,对SRIF的反应明显脱敏,而对L-362855的反应则不然。6. 当通过合并仅暴露于单一激动剂浓度的细胞的数据来获得SRIF和L-362855的浓度 - 效应曲线时,SRIF(pEC50 9.2)的效力约为L-362855(pEC50 8.0)的20倍,但最大效应相同。百日咳毒素可消除对SRIF和L-362855的反应。7. SRIF和L-362855诱导的EAR增加被N-乙基异丙基阿米洛利(10 microM)抑制,但不受蛋白激酶C抑制剂(Go-6976)、丝裂原活化蛋白激酶抑制剂(PD-98059)、酪氨酸激酶抑制剂(染料木黄酮)或酪氨酸磷酸酶抑制剂(原钒酸钠)的影响。8. 结果表明,SRIF诱导的CHOsst4细胞EAR增加涉及Na+/H+反向转运体的激活,并通过Gi/Go G蛋白介导。对SRIF而非L-362855的反应会发生明显脱敏,这可能是受体 - 效应器偶联途径差异激活的结果。