豚鼠离体胆囊中内皮素(ET)受体的特性:存在另一种ET受体亚型的证据。
Characterization of endothelin (ET) receptors in the isolated gall bladder of the guinea-pig: evidence for an additional ET receptor subtype.
作者信息
Battistini B, O'Donnell L J, Warner T D, Fournier A, Farthing M J, Vane J R
机构信息
William Harvey Research Institute, St. Bartholomew's Hospital Medical College, London.
出版信息
Br J Pharmacol. 1994 Aug;112(4):1244-50. doi: 10.1111/j.1476-5381.1994.tb13217.x.
Abstract
- We have characterized the receptors mediating contractions induced by endothelin-1 (ET-1), ET-2, ET-3 and the ETB-selective receptor agonists, sarafotoxin 6c (SX6c), IRL 1620, BQ-3020, [Ala1,3,11,15]ET-1 and ET (16-21) in strips of the isolated gall bladder of the guinea-pig (GPGB). We used as antagonists BQ-123 (ETA receptor selective) and PD 145065 (ETA/ETB receptor non-selective). 2. ET-1, ET-2 and ET-3 (10(-10) M to 3 x 10(-7) M) caused similar slowly-developing concentration-dependent contractions of the GPGB. Contractile effects induced by ET-1, ET-2 or ET-3 (at 3 x 10(-7) M) were also similar (230 +/- 25, 241 +/- 7 and 287 +/- 37% of that to histamine at 5 x 10(-6) M, n = 7, 6, 12, respectively). However, the threshold concentration for ET-1 or ET-2 was 10(-10) M whereas it was 3 x 10(-9) M for ET-3. 3. SX6c (10(-10) M to 3 x 10(-7) M) also caused slowly-developing concentration-dependent contractions at a threshold concentration of 10(-10) M (n = 16). However, the contraction caused by SX6c at 3 x 10(-7) M was 116 +/- 9% of that to histamine at 5 x 10(-6) M, which was half of that induced by the same concentration of the ET isopeptides. The contraction induced by IRL 1620 at 3 x 10-7 M (n = 9) was 43 +/- 9% of that to histamine at 5 x 10-6 M, which was one fifth of that produced by the same concentration of ET-1. Contractions induced by BQ-3020 or [Ala1,3,11,15]ET-I at 3 x 10-7 M were even less than those produced by IRL 1620. ET (16-21) was inactive up to 10-5 M. Addition of a concentration of 3 x 10-7 M of ET-1 to tissues with developed contractions induced by the bolus addition of 3 x 10-7 M SX6c caused a further contraction of the GPGB to the level observed with ET-1 alone at 3 x 10-7M (n = 8).4. BQ-123 (10-5 M) did not affect the concentration-response curve to ET-1 and the contraction induced by 3 x 10- M was also not affected (n = 5; 239 +/- 19% of histamine at 5 x 10-6 M). PD 145065(10-5 M) shifted the ET-1 concentration-response curve to the right and the contraction induced by ET-1at 3 x 10-7 M was inhibited by 15% (n = 6; NS). A higher concentration of BQ-123 (10-4 M) caused a significant shift to the right of the ET-1 concentration-response curve similar to that caused by PD 145065 (10-s M) and caused a 24% (n = 6; NS) inhibition of the contractions induced by ET-1 at 3 x 10-7 M. PD 145065 (10-4 M) abolished contractions induced by ET-1 (up to 10- M) and inhibited the response to ET-1 at 3 x 10-7 M by 52% (n = 4; P< 0.05).5. Contractions induced by ET-3 were more sensitive to inhibition by the antagonists. BQ-123 (10-6,10-5 or 10-4 M) inhibited responses to 3 x 10-7 M ET-3 by 66, 71 and 83%, respectively (n = 5, 5, 3;P< 0.05). PD 145065 (10-6, 10-5 or 10-4 M) attenuated more strongly than did BQ-123 the contractions induced by ET-3. For instance, the contractions caused by ET-3 at 3 x 10-7 M were decreased by 73 and 80% (n = 5, 5; P<0.05) in the presence of PD 145065 (10-6 or 10-5 M, respectively). PD 145065(10-4 M) completely abolished contractions to ET-3 (n = 4; up to 3 x 10-7M).6. Contractions induced by SX6c, especially those observed at concentrations lower than 10-8 M, were attenuated by BQ-123 (up to 10-4 M). PD 145065 (10-5M) shifted to the right the concentration response curve to SX6c and inhibited by 38% (P<0.05) the contractions induced by 3 x 10-7M.However, the contractions induced by a bolus addition of a high concentration of SX6c (3 x 10-7 M)and the subsequent addition of an identical concentration of ET-1 on top of SX6c were not affected byBQ-123 (10-6 or 10-5 M).7. These results suggest that ETB receptors are involved in the contractions induced by endothelins in the GPGB. However, SX6c and other selective ETB agonists produced only half or less than half of the contractile response induced by non-selective agonists. In addition, the responses to ET-1 but not to ET-3, were insensitive to the antagonist action of BQ-123 at 10-5 M whereas BQ-123 or PD 145065 at 10-5 M strongly antagonized contractions induced by ET-3. Finally, BQ-123 at 10-4 M inhibited contractions to ET-1 and SX6c. Thus, within the GPGB there may well be additional ET receptor(s) not conforming to the established ETA/ETB receptor subtype classification, as well as ETB receptors.
摘要
- 我们已对介导内皮素-1(ET-1)、ET-2、ET-3及ETB选择性受体激动剂(铃蟾毒素6c(SX6c)、IRL 1620、BQ-3020、[Ala1,3,11,15]ET-1和ET(16 - 21))在豚鼠离体胆囊条(GPGB)中引起收缩的受体进行了特性分析。我们使用BQ-123(ETA受体选择性拮抗剂)和PD 145065(ETA/ETB受体非选择性拮抗剂)作为拮抗剂。2. ET-1、ET-2和ET-3(10⁻¹⁰ M至3×10⁻⁷ M)引起GPGB类似的缓慢发展的浓度依赖性收缩。ET-1、ET-2或ET-3(3×10⁻⁷ M)诱导的收缩效应也相似(分别为5×10⁻⁶ M组胺诱导收缩的230±25%、241±7%和287±37%,n分别为7、6、12)。然而,ET-1或ET-2的阈浓度为10⁻¹⁰ M,而ET-3的阈浓度为3×10⁻⁹ M。3. SX6c(10⁻¹⁰ M至3×10⁻⁷ M)在阈浓度10⁻¹⁰ M时也引起缓慢发展的浓度依赖性收缩(n = 16)。然而,3×10⁻⁷ M的SX6c引起的收缩为5×10⁻⁶ M组胺诱导收缩的116±9%,这是相同浓度ET同工肽诱导收缩的一半。3×10⁻⁷ M的IRL 1620诱导的收缩(n = 9)为5×10⁻⁶ M组胺诱导收缩的43±9%,这是相同浓度ET-1产生收缩的五分之一。3×10⁻⁷ M的BQ-3020或[Ala1,3,11,15]ET-1诱导的收缩甚至小于IRL 1620产生的收缩。ET(16 - 21)在高达10⁻⁵ M时无活性。向预先由3×10⁻⁷ M SX6c团注诱导产生收缩的组织中添加3×10⁻⁷ M的ET-1,导致GPGB进一步收缩至单独使用3×10⁻⁷ M ET-1时观察到的水平(n = 8)。4. BQ-123(10⁻⁵ M)不影响ET-1的浓度-反应曲线,对3×10⁻⁷ M诱导的收缩也无影响(n = 5;为5×10⁻⁶ M组胺诱导收缩的239±19%)。PD 145065(10⁻⁵ M)使ET-1浓度-反应曲线右移,3×10⁻⁷ M的ET-1诱导的收缩受到15%的抑制(n = 6;无显著性差异)。更高浓度的BQ-123(10⁻⁴ M)使ET-1浓度-反应曲线显著右移,类似于PD 145065(10⁻⁵ M)引起的右移,并使3×10⁻⁷ M的ET-1诱导的收缩受到24%的抑制(n = 6;无显著性差异)。PD 145065(10⁻⁴ M)消除了ET-1诱导的收缩(高达10⁻⁷ M),并使3×10⁻⁷ M的ET-1反应受到52%的抑制(n = 4;P<0.05)。5. ET-3诱导的收缩对拮抗剂的抑制更敏感。BQ-123(10⁻⁶、10⁻⁵或10⁻⁴ M)分别抑制对3×10⁻⁷ M ET-3的反应66%、71%和83%(n分别为5、5、3;P<0.05)。PD 145065(10⁻⁶、10⁻⁵或10⁻⁴ M)比BQ-123更强烈地减弱ET-3诱导的收缩。例如,在存在PD 145065(分别为10⁻⁶或10⁻⁵ M)时,3×10⁻⁷ M的ET-3引起的收缩分别降低73%和80%(n = 5、5;P<0.05)。PD 145065(10⁻⁴ M)完全消除对ET-3的收缩(n = 4;高达3×10⁻⁷ M)。6. SX6c诱导的收缩,尤其是在浓度低于10⁻⁸ M时观察到的收缩,被BQ-123(高达10⁻⁴ M)减弱。PD 145065(10⁻⁵ M)使SX6c的浓度-反应曲线右移,并抑制3×10⁻⁷ M诱导的收缩38%(P<0.05)。然而,高浓度SX6c(3×10⁻⁷ M)团注诱导的收缩以及随后在SX6c基础上添加相同浓度ET-1诱导的收缩不受BQ-123(10⁻⁶或10⁻⁵ M)影响。7. 这些结果表明,ETB受体参与了ET在GPGB中诱导的收缩。然而,SX6c和其他选择性ETB激动剂产生的收缩反应仅为非选择性激动剂诱导收缩反应的一半或不到一半。此外,对ET-1的反应而非对ET-3的反应,对10⁻⁵ M的BQ-123拮抗剂作用不敏感,而10⁻⁵ M的BQ-123或PD 145065强烈拮抗ET-3诱导的收缩。最后,10⁻⁴ M的BQ-123抑制对ET-1和SX-6c的收缩。因此,在GPGB内可能存在不符合既定ETA/ETB受体亚型分类的其他ET受体以及ETB受体。
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