Portoghese P S, Poupaert J H, Larson D L, Groutas W C, Meitzner G D, Swenson D C, Smith G D, Duax W L
J Med Chem. 1982 Jun;25(6):684-8. doi: 10.1021/jm00348a015.
Enantiomers of erythro-5-methylmethadone (3) were synthesized from optical antipodes of erythro-3-(dimethyl-amino)-2-butanol. X-ray crystallographic analysis of (-)-3 perchlorate revealed that it possesses the 5S,6S absolute configuration. It was found that (-)-3 is substantially more potent than its enantiomer (+)-3 as an opioid agonist in vivo and in vitro. In vitro tests (guinea pig ileal longitudinal muscle and mouse vas deferens preparations) suggest that (-)-3 mediates its effect chiefly through mu opioid receptors. On the other hand, (+)-3 and the more potent enantiomers of methadone, (-)-1, and isomethadone, (-)-2, appear to have less mu-receptor selectivity and interact with a greater fraction of delta receptors than does (-)-3. The fact that the solid-state conformation of (-)-3 differs from that of (-)-1 and (-)-2, which show great similarity in conformational features, suggests that mu and delta receptors have different conformational requirements. The possibility of different modes of interaction with a single opioid receptor population also is discussed.
从赤藓糖型-3-(二甲氨基)-2-丁醇的旋光对映体合成了赤藓糖型-5-甲基美沙酮(3)的对映体。对(-)-3高氯酸盐进行X射线晶体学分析表明,它具有5S,6S绝对构型。研究发现,(-)-3作为阿片类激动剂在体内和体外的效力明显高于其对映体(+)-3。体外试验(豚鼠回肠纵肌和小鼠输精管制剂)表明,(-)-3主要通过μ阿片受体介导其作用。另一方面,(+)-3以及美沙酮更有效的对映体(-)-1和异美沙酮(-)-2似乎对μ受体的选择性较低,与δ受体相互作用的比例比(-)-3更大。(-)-3的固态构象与(-)-1和(-)-2不同,后两者在构象特征上有很大相似性,这一事实表明μ和δ受体有不同的构象要求。还讨论了与单一阿片受体群体相互作用的不同模式的可能性。
