豚鼠离体小肠纵肌对血管紧张素类似物收缩反应的药理学特性
Pharmacological characterization of the contractile responses to angiotensin analogues in guinea-pig isolated longitudinal muscle of small intestine.
作者信息
Hawcock A B, Barnes J C
机构信息
Neuropharmacology Department, Glaxo Group Research Ltd., Ware, Hertfordshire.
出版信息
Br J Pharmacol. 1993 Apr;108(4):1150-5. doi: 10.1111/j.1476-5381.1993.tb13519.x.
Abstract
- The contractile responses to angiotensin II, angiotensin III and two synthetic analogues, [Lys2]angiotensin II and [Sar1]angiotensin II, in the guinea-pig isolated longitudinal muscle preparation of small intestine have been characterized in vitro. 2. Tachyphylaxis to the angiotensin analogues was reduced by use of a Krebs-Henseleit solution containing a raised (sub-contractile) concentration of potassium (11.2 mM). Under these conditions. reproducible cumulative concentration-response curves to all agonists were established. The pD2 estimates for angiotensin II, [Lys2]angiotensin II, angiotensin III and [Sar1]angiotensin II were 9.15 +/- 0.14, 7.42 +/- 0.06, 7.69 +/- 0.18 and 9.50 +/- 0.15 respectively and the maximum responses achieved were not significantly different. 3. The contractile responses to angiotensin II, angiotensin III and [Sar1]angiotensin II were reduced by greater than 80% by tetrodotoxin (TTX; 0.1 microM). However, the responses to [Lys2]angiotensin II were reduced by only 63 +/- 5%. Atropine (0.1 microM) also reduced the responses to angiotensin II, angiotensin III and [Lys2]angiotensin II, although its effect was less than that produced by TTX. Furthermore, while responses to these agonists were not significantly modified by the NK1 receptor antagonist (+/-)-CP-96,345 (30 nM) alone, the combined pre-incubation with both atropine and (+/-)-CP-96,345 reduced maximum agonist responses to a level not significantly different from those produced by TTX. 4. Indirect and direct contractile responses to angiotensin II and [Lys2]angiotensin II (in the presence of TTX) respectively were characterized by use of the selective AT1 receptor antagonist, losartan and the AT2 receptor antagonist, PD123177. Losartan produced parallel rightward displacement of the concentration-response curve to angiotensin II and [Lys2]angiotensin II, with an estimated pKB of 8.56(8.42-8.68) and 9.18 (8.63-9.50) respectively. The AT2 receptor antagonist, PD123177 (3 microM) failed to modify the contractile responses to either angiotensin II or [Lys2]angiotensin II.5. We conclude that two populations of angiotensin II receptors exist in the guinea-pig longitudinal muscle of small intestine, one located neuronally mediating the release of both acetylcholine and substance P and the other located on the smooth muscle mediating direct contractile responses. The neuronal component provides the major contribution to the agonist responses. Both receptor populations are of the AT1 receptor subtype.
摘要
- 已在体外对豚鼠离体小肠纵肌标本中血管紧张素II、血管紧张素III以及两种合成类似物[Lys2]血管紧张素II和[Sar1]血管紧张素II的收缩反应进行了表征。2. 通过使用含有升高(亚收缩)浓度钾(11.2 mM)的克雷布斯 - 亨塞尔特溶液,可减轻对血管紧张素类似物的快速耐受性。在这些条件下,建立了对所有激动剂的可重复的累积浓度 - 反应曲线。血管紧张素II、[Lys2]血管紧张素II、血管紧张素III和[Sar1]血管紧张素II的pD2估计值分别为9.15±0.14、7.42±0.06、7.69±0.18和9.50±0.15,且达到的最大反应无显著差异。3. 河豚毒素(TTX;0.1 microM)使对血管紧张素II、血管紧张素III和[Sar1]血管紧张素II的收缩反应降低超过80%。然而,对[Lys2]血管紧张素II的反应仅降低63±5%。阿托品(0.1 microM)也降低了对血管紧张素II、血管紧张素III和[Lys2]血管紧张素II的反应,尽管其作用小于TTX产生的作用。此外,虽然单独使用NK1受体拮抗剂(+/-)-CP - 96,345(30 nM)对这些激动剂的反应无显著影响,但与阿托品和(+/-)-CP - 96,345联合预孵育可将最大激动剂反应降低至与TTX产生的反应无显著差异的水平。4. 通过使用选择性AT1受体拮抗剂氯沙坦和AT2受体拮抗剂PD123177,分别表征了对血管紧张素II和[Lys2]血管紧张素II(在TTX存在下)的间接和直接收缩反应。氯沙坦使血管紧张素II和[Lys2]血管紧张素II的浓度 - 反应曲线平行向右位移,估计的pKB分别为8.56(8.42 - 8.68)和9.18(8.63 - 9.50)。AT2受体拮抗剂PD123177(3 microM)未能改变对血管紧张素II或[Lys2]血管紧张素II的收缩反应。5. 我们得出结论,豚鼠小肠纵肌中存在两种血管紧张素II受体群体,一种位于神经元上,介导乙酰胆碱和P物质的释放,另一种位于平滑肌上,介导直接收缩反应。神经元成分对激动剂反应起主要作用。两种受体群体均为AT1受体亚型。
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