凝血酶受体衍生多肽的血管作用:大鼠主动脉收缩和舒张作用的构效关系
Vascular actions of thrombin receptor-derived polypeptides: structure-activity profiles for contractile and relaxant effects in rat aorta.
作者信息
Laniyonu A A, Hollenberg M D
机构信息
Department of Pharmacology & Therapeutics, University of Calgary, Faculty of Medicine, AB Canada.
出版信息
Br J Pharmacol. 1995 Apr;114(8):1680-6. doi: 10.1111/j.1476-5381.1995.tb14957.x.
Abstract
- Using endothelium-denuded and intact rat aortic rings, we have determined the contractile and relaxant structure-activity profile for a series of thrombin receptor-derived polypeptides (TRPs) based on the human and rat receptor sequences: SFLLR (P5), SFLLR-NH2 (P5-NH2) SFFLR (Rat P5), SFFLR-NH2 (Rat P5-NH2), SFLLRNP (P7), SFLLRNP-NH2 (P7-NH2), SFFLRNP (Rat P7), SFFLRNP-NH2 (Rat P7-NH2), and SFLLRNPNDKYEPF (P14). 2. A contractile response to thrombin and the TRPs in the endothelium-denuded aortic tissue was minimal or absent in preparations obtained from animal weighing less than 180 g (< 6 weeks of age), but increased with animal size, plateauing in tissues derived from animals weighing between 320 and 420 g (about 9 to 14 weeks of age). In contrast, the contractile responses to KCl and noradrenaline did not differ in the tissues and relaxant responses to the TRPs in endothelium-intact aortic preparations were comparable for tissues obtained from either young (< or = 180 g) or older (> or = 320 g) animals. 3. The contractile response of the endothelium-denuded preparation to thrombin and the TRPs showed marked cross-desensitization: the relaxation response of the intact rings did not desensitize to the TRPs. 4. The relative potencies for the TRPs in the aortic contraction assay were comparable to those for the relaxation assay, but were distinct from the relative potencies we measured previously in a rat gastric longitudinal muscle contraction assay. Further, P5 behaved as a partial agonist in the aortic contraction assay, whereas it had been observed to be a full agonist in the gastric contraction assay. 5. The contractile activity of P5-NH2 in endothelium intact aortic rings was low or absent, but in the presence of the nitric oxide synthase inhibitor, N omega-nitro-L-arginine-methyl ester (L-NAME), the contractions in the intact preparation were equivalent to the response of the endothelium-denuded preparation in the absence of L-NAME.6. The contractile response of the endothelium-denuded aortic preparation to P5-NH2 was inhibited by nifedipine and the kinase C antagonist, chelerythrine, but was resistant to the action of indomethacin,tetrodotoxin and the tyrosine kinase inhibitor, genistein.7 We conclude that the receptor system for the TRPs in the aortic smooth muscle elements, responsible for the contractile response, is similar to the aortic endothelial cell receptor responsible for the relaxation response, but is distinct from the receptor that we have previously characterized in gastric longitudinal smooth muscle, results pointing to the presence of receptor subtypes in the vascular and gastric smooth muscle elements.
摘要
我们使用去内皮和完整的大鼠主动脉环,基于人和大鼠受体序列确定了一系列凝血酶受体衍生多肽(TRP)的收缩和舒张结构 - 活性概况:SFLLR(P5)、SFLLR - NH₂(P5 - NH₂)、SFFLR(大鼠P5)、SFFLR - NH₂(大鼠P5 - NH₂)、SFLLRNP(P7)、SFLLRNP - NH₂(P7 - NH₂)、SFFLRNP(大鼠P7)、SFFLRNP - NH₂(大鼠P7 - NH₂)以及SFLLRNPNDKYEPF(P14)。
对体重小于180克(小于6周龄)动物制备的去内皮主动脉组织,凝血酶和TRP引起的收缩反应极小或不存在,但随动物体型增大而增加,在体重320至420克(约9至14周龄)动物的组织中达到平稳状态。相反,去内皮组织对氯化钾和去甲肾上腺素的收缩反应以及完整主动脉制剂中TRP引起的舒张反应在年轻(≤180克)或年老(≥320克)动物获得的组织中相当。
去内皮制剂对凝血酶和TRP的收缩反应表现出明显的交叉脱敏:完整环的舒张反应对TRP不会脱敏。
在主动脉收缩试验中TRP的相对效力与舒张试验中的相当,但与我们之前在大鼠胃纵肌收缩试验中测得的相对效力不同。此外,P5在主动脉收缩试验中表现为部分激动剂,而在胃收缩试验中曾观察到它是完全激动剂。
P5 - NH₂在完整内皮主动脉环中的收缩活性低或不存在,但在一氧化氮合酶抑制剂Nω - 硝基 - L - 精氨酸甲酯(L - NAME)存在时,完整制剂中的收缩与不存在L - NAME时去内皮制剂的反应相当。
去内皮主动脉制剂对P5 - NH₂的收缩反应被硝苯地平和蛋白激酶C拮抗剂白屈菜红碱抑制,但对吲哚美辛、河豚毒素和酪氨酸激酶抑制剂染料木黄酮的作用有抗性。
我们得出结论,主动脉平滑肌元件中负责收缩反应的TRP受体系统与负责舒张反应的主动脉内皮细胞受体相似,但与我们之前在胃纵肌中鉴定的受体不同,结果表明血管和平滑肌元件中存在受体亚型。
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