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Endothelin receptor expression and pharmacology in human saphenous vein graft

机译:人体大隐静脉移植物中内皮素受体的表达和药理作用

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摘要

We have investigated the expression and pharmacology of endothelin (ET) receptors in human aortocoronary saphenous vein grafts.Subtype-selective ligands were used to autoradiographically identify ETA ([125I]-PD151242) and ETB ([125I]-BQ3020) receptors. In graft saphenous vein ETA receptors predominated in the media, with few ETB receptors identified. Neither subtype was detected in the thickened neointima.The ratio of medial ETA:ETB receptors was 75% : 25% in both graft and control saphenous vein.ET-1 contracted control (EC50 2.9 nM) and graft (EC50 4.5 nM) saphenous vein more potently than diseased coronary artery (EC50 25.5 nM).In all three blood vessels ET-1 was 100 times more potent than ET-3 and three times more potent than sarafotoxin 6b (S6b). Little or no response was obtained in any vessel with the ETB agonist sarafotoxin 6c (S6c).The ETA antagonist PD156707 (100 nM) blocked ET-1 responses in all three vessels with pKb values of approximately 8.0.For individual graft veins the EC50 value for ET-1 and ‘age' of graft in years showed a significant negative correlation.In conclusion there is no alteration in ET receptor expression in the media of saphenous veins grafted into the coronary circulation compared to control veins. ETA receptors predominantly mediate the vasoconstrictor response to ET-1 in graft vein, with no apparent up-regulation of ETB receptors. The sensitivity of the graft vein to ET-1 increased with graft ‘age', suggesting that these vessels may be particularly vulnerable to the increased plasma ET levels that are detected in patients with cardiovascular disease.
机译:我们已经研究了内皮素(ET)受体在人主动脉冠状大隐静脉移植物中的表达和药理作用。亚型选择性配体用于放射自显影识别ETA([125I] -PD151242)和ETB([125I] -BQ3020)受体。在移植大隐静脉中,ETA受体在培养基中占主导地位,几乎没有ETB受体被发现。在增厚的新内膜中均未检测到亚型。在移植和对照隐静脉中,ETA:ETB内侧受体的比例为75%:25%.ET-1收缩了对照(EC50 2.9 nM)和移植物(EC50 4.5 nM)隐静脉。比患病的冠状动脉(EC50 25.5nM)更有效。在所有三个血管中,ET-1的效力比ET-3高100倍,比sarafotoxin 6b(S6b)强3倍。用ETB激动剂sarafotoxin 6c(S6c)在任何血管中几乎没有反应,甚至没有反应.ETA拮抗剂PD156707(100 nM)在所有三个血管中均阻断了ET-1反应,pKb值约为8.0。对于单个移植静脉,EC50值ET-1与移植物的“年龄”之间存在显着的负相关。总之,与对照静脉相比,在移植到冠脉循环中的大隐静脉的介质中ET受体的表达没有改变。 ETA受体主要介导移植静脉中对ET-1的血管收缩反应,而ETB受体没有明显的上调。移植物静脉对ET-1的敏感性随移植物“年龄”的增加而增加,这表明这些血管可能特别易受心血管疾病患者血浆ET水平升高的影响。

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