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介导豚鼠气管速激肽诱导收缩反应的受体。

Receptors mediating tachykinin-induced contractile responses in guinea-pig trachea.

作者信息

Ireland S J, Bailey F, Cook A, Hagan R M, Jordan C C, Stephens-Smith M L

机构信息

Department of Neuropharmacology, Glaxo Group Research Ltd., Hertfordshire.

出版信息

Br J Pharmacol. 1991 Jun;103(2):1463-9. doi: 10.1111/j.1476-5381.1991.tb09812.x.

Abstract
  1. The classification of tachykinin receptors in the guinea-pig trachea has been investigated. This was of interest because, from previous studies, it was not clear whether the guinea-pig trachea contains either a mixture of NK1 and NK2 receptors or, alternatively, a single type of novel tachykinin receptor. 2. In the present study, the guinea-pig trachea was contracted by tachykinin agonists selective for NK1 receptors (substance P methylester (SPOMe) and GR73632) or NK2 receptors (GR64349) but not NK3 receptors (senktide). 3. Against SPOMe and GR73632, the NK1 antagonist, GR71251, behaved as a reversible competitive antagonist having apparent affinity (pKB 7.05 vs SPOMe) consistent with action at NK1 receptors. GR71251 (3 microM) did not antagonize responses to GR64349. 4. The NK2 antagonists L-659,877 and Ac-Leu-Asp-Gln-Trp-Phe-Gly-NH2 (R396) antagonized GR64349 although only R396 appeared to behave competitively (pKB 5.73). Neither L-659,877 (30 microM) nor R396 (30 microM) blocked responses to SPOMe. 5. For L-659,877 and R396, comparison was made between activity in guinea-pig trachea and in preparations known to contain tachykinin receptors predominantly of the NK2 type. In the rabbit trachea, both L-659,877 and R396 had effects similar to those in guinea-pig trachea. In contrast, in the rat colon muscularis mucosae, both L-659,877 and R396 appeared to behave competitively with pKB values against GR64349 of 7.83 and 6.90 respectively. 6. It is concluded that in guinea-pig trachea, contractile responses can be induced by activation of both NK1 and NK2 receptors. The present data are discussed with reference to the proposed existence of subtypes of the NK2 receptor.
摘要
  1. 对豚鼠气管中速激肽受体的分类进行了研究。这一点很有意思,因为根据之前的研究,尚不清楚豚鼠气管中是含有NK1和NK2受体的混合物,还是一种单一类型的新型速激肽受体。2. 在本研究中,豚鼠气管被对NK1受体有选择性的速激肽激动剂(P物质甲酯(SPOMe)和GR73632)或NK2受体(GR64349)而非NK3受体(速激肽)收缩。3. 对于SPOMe和GR73632,NK1拮抗剂GR71251表现为可逆竞争性拮抗剂,其表观亲和力(与SPOMe相比pKB为7.05)与作用于NK1受体一致。GR71251(3 microM)不拮抗对GR64349的反应。4. NK2拮抗剂L-659,877和Ac-Leu-Asp-Gln-Trp-Phe-Gly-NH2(R396)拮抗GR64349,尽管只有R396表现出竞争性(pKB为5.73)。L-659,877(30 microM)和R396(30 microM)均不阻断对SPOMe的反应。5. 对于L-659,877和R396,比较了它们在豚鼠气管和已知主要含有NK2型速激肽受体的制剂中的活性。在兔气管中,L-659,877和R396的作用与在豚鼠气管中的作用相似。相比之下,在大鼠结肠肌黏膜中,L-659,877和R396似乎都表现出竞争性,对GR64349的pKB值分别为7.83和6.90。6. 得出结论,在豚鼠气管中,NK1和NK2受体的激活均可诱导收缩反应。结合NK2受体亚型的假定存在对目前的数据进行了讨论。

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