Meini S, Patacchini R, Lecci A, Poulos C, Rovero P, Maggi C A
Pharmacology Department, A. Menarini Pharmaceuticals, Florence, Italy.
Neuropeptides. 1995 Feb;28(2):99-106. doi: 10.1016/0143-4179(95)90081-0.
The existence of a septide-sensitive subtype of the tachykinin NK1 receptor has been recently proposed. In the rat isolated urinary bladder, the non-peptide NK1 receptor antagonist RP 67,580 exhibits a higher affinity towards septide (pKB 7.57) than towards [Sar9]substance P sulfone (pKB 7.00). In this study we have investigated the pharmacological profile of the non-mammalian tachykinin physalaemin, of the synthetic NK1 receptor agonist GR 73,632 (delta-aminovaleryl[LPro9,NMeLeu10]substance P(7-11)) and of [Glu(OBzl)11]substance P in relation to the putative existence of a septide-sensitive receptor. The activity of [Glu(OBzl)11]substance P at the NK1, NK2 and NK3 receptor was assayed in the guinea-pig ileum NK1 receptor assay (EC50 26 nM), in the rabbit pulmonary artery NK2 receptor assay (weak agonist activity) and in the rat portal vein NK3 receptor assays (no appreciable activity up to 1 microM). GR 73,632, [Glu(OBzl)11]substance P and physalaemin, all produced concentration-dependent contractions of the rat isolated urinary bladder, with EC50 values of 17, 79, and 9 nM, respectively. The responses to the three agonists were very slightly or not modified by the NK2 receptor antagonist SR 48,968 (1 microM). RP 67,580 (0.3-3 microM) produced a concentration-dependent rightward shift of the curve to GR 73,632, [Glu(OBzl)11]substance P and physalaemin without producing depression of their maximal response. Schild plot analysis indicated the competitive nature of the antagonism. The affinity (pKB) of RP 67,580 towards physalaemin, GR 73,632 and [Glu(OBzl)11]substance P was 7.12, 7.56 and 7.95, respectively.(ABSTRACT TRUNCATED AT 250 WORDS)
最近有人提出速激肽NK1受体存在对七肽敏感的亚型。在大鼠离体膀胱中,非肽类NK1受体拮抗剂RP 67,580对七肽(pKB 7.57)的亲和力高于对[Sar9]P物质砜(pKB 7.00)的亲和力。在本研究中,我们研究了非哺乳动物速激肽 Physalaemin、合成的NK1受体激动剂GR 73,632(δ-氨基戊酰基[LPro9,NMeLeu10]P物质(7 - 11))以及[Glu(OBzl)11]P物质与假定存在的对七肽敏感受体相关的药理学特性。在豚鼠回肠NK1受体试验(EC50 26 nM)、兔肺动脉NK2受体试验(弱激动剂活性)和大鼠门静脉NK3受体试验(高达1 μM无明显活性)中测定了[Glu(OBzl)11]P物质在NK1、NK2和NK3受体上的活性。GR 73,632、[Glu(OBzl)11]P物质和 Physalaemin均使大鼠离体膀胱产生浓度依赖性收缩,EC50值分别为17、79和9 nM。NK2受体拮抗剂SR 48,968(1 μM)对这三种激动剂的反应影响非常轻微或无影响。RP 67,580(0.3 - 3 μM)使GR 73,632、[Glu(OBzl)11]P物质和 Physalaemin的剂量反应曲线浓度依赖性右移,但其最大反应未受抑制。Schild图分析表明拮抗作用具有竞争性。RP 67,580对 Physalaemin、GR 73,632和[Glu(OBzl)11]P物质的亲和力(pKB)分别为7.12、7.56和7.95。(摘要截短于250字)
