[Pharmacology of the venous system].

Journal de pharmacologie Pub Date : 1986-01-01
J van den Driessche, D Milon, B Saiag
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引用次数: 0

Abstract

The presence of alpha 1-receptors has been demonstrated in numerous venous fragments for various animal models. On the other hand, the presence of alpha 2-receptors in the saphenous of the dog is a matter of debate. Beta 2-receptors are activated by isoproterenol, noradrenaline and adrenaline in precontracted veins (part of the facial vein of the rabbit may be an exception). Preferential blocking by atenolol of beta 1-receptors in the jugular veins of the rat suggests that these receptors may mediate vasodilation. The saphenous veins of the dog provide the only example where specific dopaminergic receptors have been noted following partial antagonism with haloperidol. The vasoconstrictive action of acetylcholine has been seen in venous segments of numerous species and indicates the presence of muscarinic receptors. The existence of angiotensin receptors can be postulated despite the weak and inconstant in vitro and in vivo (the dorsal cerebral sinus in the dog excepted) reactions observed and the use of a non-specific antagonist. The same is true for bradykinin and vasopressin. The marked vasoconstrictive action of serotonin on all veins studied is evidence for the presence of receptors. The nature of the antagonists is subject to some divergence of opinion. Nevertheless, D tryptamine muscular receptors (or 5 HT2) can be identified due to the lack of morphine-mediated response and the efficacy of methysergide. The presence of a third type of serotoninergic receptor has only been reported once, following observations of vasodilation in the sheep. H1 receptors are involved in histamine-mediated vasoconstriction. The presence of H2 receptors which mediate vasodilation in precontracted veins remains hypothetical. Prostaglandins exhibit different efficacies in producing contraction in isolated veins; PGF2 alpha is more efficacious than PGE1 and PGE2. Prostacyclin induces contraction of human saphenous veins in a dose-dependent manner. PGE2 and particularly PGE1 can induce relaxation in precontracted veins, as is also true for prostacyclin. Receptors for these prostaglandins must exist at the post-junctional level. P2-receptors mediate transmission of the vasoconstrictive action of various purine derivatives.

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[静脉系统药理学]。
α - 1受体的存在已经在许多动物模型的静脉片段中得到证实。另一方面,α 2受体在狗的隐静脉中的存在是一个有争议的问题。β 2受体被异丙肾上腺素、去甲肾上腺素和预收缩静脉中的肾上腺素激活(家兔部分面部静脉可能是个例外)。阿替洛尔对大鼠颈静脉β 1受体的优先阻断表明这些受体可能介导血管舒张。狗的隐静脉提供了唯一的例子,其中特定的多巴胺能受体已注意到与氟哌啶醇部分拮抗。乙酰胆碱的血管收缩作用已在许多物种的静脉段中发现,表明存在毒蕈碱受体。尽管在体外和体内(狗的脑背窦除外)观察到的反应较弱且不稳定,并且使用了非特异性拮抗剂,但可以假设血管紧张素受体的存在。缓激素和抗利尿激素也是如此。血清素对所有静脉的显著收缩作用是受体存在的证据。对立双方的性质存在一些意见分歧。然而,由于缺乏吗啡介导的反应和甲基塞吉特的疗效,可以确定D -色胺肌肉受体(或5ht2)。第三种类型的血清素受体的存在只报道了一次,在绵羊血管舒张的观察。H1受体参与组胺介导的血管收缩。H2受体在预收缩静脉中介导血管扩张的存在仍然是假设的。前列腺素在离体静脉收缩中表现出不同的效果;PGF2 α比PGE1和PGE2更有效。前列环素以剂量依赖的方式诱导人隐静脉收缩。PGE2,特别是PGE1可以诱导预收缩静脉松弛,前列环素也是如此。这些前列腺素的受体必须存在于结膜后水平。p2受体介导各种嘌呤衍生物的血管收缩作用的传递。
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