豚鼠盲肠带中嘌呤受体激动剂与拮抗剂相互作用的药理学分析。

Pharmacological analysis of the interaction between purinoceptor agonists and antagonists in the guinea-pig taenia caecum.

作者信息

Prentice D J, Shankley N P, Black J W

机构信息

Department of Analytical Pharmacology, Rayne Institute, King's College Hospital School of Medicine and Dentistry, London.

出版信息

Br J Pharmacol. 1995 Jun;115(4):549-56. doi: 10.1111/j.1476-5381.1995.tb14967.x.

DOI:10.1111/j.1476-5381.1995.tb14967.x

PMID:7582471

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1908477/

Abstract

In the absence of adenosine uptake inhibition, adenosine produced a concentration-dependent (threshold 30 microM) relaxation of the 5-methylfurmethide pre-contracted guinea-pig taenia caecum. The relaxation was not blocked by 8-phenyltheophylline (8-PT, 3 microM) or 1,3-dipropyl, 8-cyclopentylxanthine (DPCPX, 30 microM). 2. In the presence of the adenosine uptake inhibitor, dipyridamole (Dip, 3 microM), a biphasic adenosine concentration-effect curve was obtained (threshold 0.3 microM). The time course of the responses to adenosine in the absence of Dip was similar to that of the second phase responses in the presence of Dip and occurred over the same adenosine concentration-range. 5'-(N-ethyl) carboxamido-adenosine (NECA) concentration-effect curves (in the absence of Dip) were also biphasic. Only the first phases of the concentration-effect curves obtained with NECA and adenosine (plus Dip) were inhibited by 8-PT. The pA2 values for 8-PT of 6.7 and 7.0 versus adenosine and NECA, respectively, were consistent with actions at P1-purinoceptors. There was a trend towards an increase in the upper asymptote of the first phase of the NECA curve in the presence of increasing concentrations of 8-PT. The A1-purinoceptor selective antagonist, DPCPX, also blocked only the first phase of the NECA concentration-effect curve and produced a significant increase in the upper asymptote. The pA2 value (6.8) obtained was consistent with activation of A2-subtype P1-purinoceptors by the low concentrations of NECA. 3. There was no correlation between A1-purinoceptor affinity and the propensity to cause the increase in the upper asymptote of the first phase of the NECA concentration-effect curves amongst a series of 9-methyl adenine analogues, suggesting that the amplification was not due to inhibition of an underlying A1-purinoceptor-mediated contractile response.4. DPCPX (10 microM) produced a significant increase in the upper asymptote of the NECA concentration effect curve, but had no effect on isoprenaline curves whereas the phosphodiesterase inhibitor Ro20-1724 (30 microM) produced a significant increase in the upper asymptote of both NECA and isoprenaline concentration-effect curves. Therefore the amplification of the first phase responses by DPCPX did not appear to be due to phosphodiesterase inhibition.5. It was not possible to conclude whether second phase responses to adenosine and NECA were mediated by intracellular or extracellular sites of action. However, if intracellular sites of action were involved then adenosine did not apparently gain access by the Dip-sensitive uptake system.

摘要

在不存在腺苷摄取抑制的情况下，腺苷对5-甲基糠甲胺预收缩的豚鼠盲肠绦虫产生浓度依赖性（阈值为30微摩尔）的舒张作用。该舒张作用不被8-苯基茶碱（8-PT，3微摩尔）或1,3-二丙基-8-环戊基黄嘌呤（DPCPX，30微摩尔）阻断。2. 在存在腺苷摄取抑制剂双嘧达莫（Dip，3微摩尔）的情况下，获得了双相的腺苷浓度-效应曲线（阈值为0.3微摩尔）。在不存在Dip时对腺苷反应的时间进程与存在Dip时第二相反应的时间进程相似，且发生在相同的腺苷浓度范围内。5'-(N-乙基)羧酰胺腺苷（NECA）的浓度-效应曲线（在不存在Dip时）也是双相的。仅NECA和腺苷（加Dip）获得的浓度-效应曲线的第一相被8-PT抑制。8-PT对腺苷和NECA的pA2值分别为6.7和7.0，这与作用于P1嘌呤受体一致。在存在浓度递增的8-PT时，NECA曲线第一相的上渐近线有增加的趋势。A1嘌呤受体选择性拮抗剂DPCPX也仅阻断NECA浓度-效应曲线的第一相，并使上渐近线显著增加。获得的pA2值（6.8）与低浓度NECA激活A2亚型P1嘌呤受体一致。3. 在一系列9-甲基腺嘌呤类似物中，A1嘌呤受体亲和力与引起NECA浓度-效应曲线第一相上渐近线增加的倾向之间没有相关性，这表明这种放大不是由于抑制潜在的A1嘌呤受体介导的收缩反应。4. DPCPX（10微摩尔）使NECA浓度效应曲线的上渐近线显著增加，但对异丙肾上腺素曲线无影响，而磷酸二酯酶抑制剂Ro20-1724（30微摩尔）使NECA和异丙肾上腺素浓度-效应曲线的上渐近线均显著增加。因此，DPCPX对第一相反应的放大似乎不是由于磷酸二酯酶抑制。5. 无法确定对腺苷和NECA的第二相反应是由细胞内还是细胞外作用位点介导的。然而，如果涉及细胞内作用位点，那么腺苷显然不是通过Dip敏感的摄取系统进入的。