Pertz H H, Brown A M, Gager T L, Kaumann A J
Fachbereich Pharmazie, Freie Universität Berlin, Germany.
J Pharm Pharmacol. 1999 Mar;51(3):319-30. doi: 10.1211/0022357991772321.
A series of simple O-acylated derivatives of the naturally occurring clavine alkaloids lysergol and dihydrolysergol-I were synthesized and tested in-vitro for their ability to interact with 5-HT2A receptors in rat tail artery, 5-HT2C receptors in piglet choroid plexus, 5-HT1B receptors in guinea-pig iliac artery and alpha1-adrenergic receptors in rat aorta. In contrast to the classical ergoline 5-HT2A receptor antagonists methysergide and LY53857, the compounds produced competitive antagonism of the 5-HT response in rat tail artery. Affinities of ergolines 3-14 were higher (pA2 values of 7.33-8.40) than those of the parent alcohols lysergol (1) and dihydrolysergol-I (2), respectively. The introduction of an isopropyl substituent at the N(1) position of the compounds failed to enhance 5-HT2A receptor affinity. Compounds 3-14 exhibited lower affinities for alpha1-adrenergic receptors than for 5-HT2A receptors. In particular, those lysergol derivatives that had an isopropyl substituent at the N(1) position were highly specific 5-HT2A receptor antagonists (ratio 5-HT2A/alpha1 = 302-3548). Selected derivatives of lysergol (3-5, 9-11) which were assayed for radioligand binding at 5-HT2C receptors in piglet choroid plexus had affinities that were similar to those found in rat tail artery. Additionally, lysergol and its N(1)-unsubstituted derivatives were found to be partial agonists (alpha of 0.2-0.4) for 5-HT2C receptor-mediated inositol phosphate accumulation in piglet choroid plexus. On the other hand, analogues with an isopropyl substituent at N(1) showed no measurable agonist activity. The observation that N(1)-unsubstituted derivatives of lysergol possessed agonist properties at 5-HT2C receptors whereas their agonist activity at 5-HT2A receptors was marginal (alpha of 0.05 for compound 3 at 1 microM) or not measurable, suggests that these compounds have different abilities to cause conformational change at the two receptor types. Selected derivatives of lysergol (3-5, 9-11) which were examined as ligands for 5-HT1B receptors in guinea-pig iliac artery caused insurmountable blockade of the contractile effect of 5-HT. N(1)-isopropyl derivatives had 30-50-fold lower affinities for 5-HT1B receptors of this tissue than their N(1)-unsubstituted analogues. It is concluded that O-acylated derivatives of the clavine alkaloids lysergol and dihydrolysergol-I mimic therapeutically relevant ergolines due to the complexity of their pharmacological profile as partial agonists and antagonists at 5-HT2A, 5-HT2C and 5-HT1B receptors, and at alpha1-adrenergic receptors.
合成了一系列天然存在的麦角灵生物碱麦角醇和二氢麦角醇 -I 的简单 O - 酰化衍生物,并在体外测试了它们与大鼠尾动脉中的 5 - HT2A 受体、仔猪脉络丛中的 5 - HT2C 受体、豚鼠髂动脉中的 5 - HT1B 受体以及大鼠主动脉中的 α1 - 肾上腺素能受体相互作用的能力。与经典的麦角灵 5 - HT2A 受体拮抗剂甲基麦角新碱和 LY53857 不同,这些化合物对大鼠尾动脉中的 5 - HT 反应产生竞争性拮抗作用。麦角灵 3 - 14 的亲和力(pA2 值为 7.33 - 8.40)分别高于母体醇麦角醇(1)和二氢麦角醇 -I(2)。在化合物的 N(1) 位引入异丙基取代基未能增强 5 - HT2A 受体亲和力。化合物 3 - 14 对 α1 - 肾上腺素能受体的亲和力低于对 5 - HT2A 受体的亲和力。特别是,那些在 N(1) 位有异丙基取代基的麦角醇衍生物是高度特异性的 5 - HT2A 受体拮抗剂(5 - HT2A/α1 比值为 302 - 3548)。在仔猪脉络丛中对 5 - HT2C 受体进行放射性配体结合测定的麦角醇选定衍生物(3 - 5,9 - 11)的亲和力与在大鼠尾动脉中发现的相似。此外,发现麦角醇及其 N(1) - 未取代衍生物是仔猪脉络丛中 5 - HT2C 受体介导的肌醇磷酸积累的部分激动剂(α 值为 0.2 - 0.4)。另一方面,在 N(1) 位有异丙基取代基的类似物未显示出可测量的激动剂活性。麦角醇的 N(1) - 未取代衍生物在 5 - HT2C 受体上具有激动剂特性,而它们在 5 - HT2A 受体上的激动剂活性微弱(化合物 3 在
