Brine G A, Stark P A, Liu Y, Carroll F I, Singh P, Xu H, Rothman R B
Research Triangle Institute, Research Triangle Park, North Carolina 27709, USA.
J Med Chem. 1995 Apr 28;38(9):1547-57. doi: 10.1021/jm00009a015.
(+/-)-cis-N-[1-(2-Hydroxy-2-phenylethyl)-3-methyl-4-piperidyl]-N- phenylpropanamide (1) is a mixture of four stereoisomers [(2S,3R,4S)-1a, (2R,3R,4S)-1b, (2R,3S,4R)-1c, and (2S,3S,4R)-1d], which together constitute two diastereoisomeric pairs of optical isomers. These four stereoisomers were prepared from optically active intermediates of known absolute configuration by procedures which had no effect on the configurations of the piperidine 3- and 4-carbons. The configuration of the phenylethyl 2-carbon in the final products was determined by X-ray analysis of (2S,3S,4R)-1d. A 1H NMR comparison of the final products to ohmefentanyl established that the racemic pair previously known as ohmefentanyl was a mixture of (2S,3R,4S)-1a and (2R,3S,4R)-1c. The individual activities of 1a, 1b, 1c, and 1d were evaluated in a variety of binding and pharmacological assays. The binding data revealed that isomers 1b and 1c had the highest affinity and selectivity for the mu site labeled with [3H]DAMGO. In contrast, the four isomers displaced [3H]etorphine in the order 1a approximately 1b > 1c approximately 1d. Evaluation of the four isomers on the mouse vas deferens (MVD) preparation revealed a potency order of 1a > 1b > 1c > 1d with concentrations of 1a and 1b in the femtomolar range causing inhibition. Experiments using the antagonists naltrexone (mu), ICI 174864 (delta), and norbinaltorphimine (kappa) demonstrated that the effects of 1a were mediated largely by the mu receptor while both delta and kappa agonist effects contributed to the actions of 1b and 1c. Isomer 1d acted as a weak mu antagonist in the MVD preparation. The same potency order was observed in a mouse analgesic assay and a rhesus monkey single dose suppression study. From the latter study the potency of 1a was estimated to be 20,000-50,000 times that of morphine, making this isomer one of the most potent opiates known. In the rhesus monkey study, isomer 1d failed to substitute for morphine and seemed to exacerbate withdrawal at doses of 0.6, 3.0, and 6.0 mg/kg. On the basis of the mouse data, isomer 1a was 21,000 times more potent than 1d, whereas isomers 1b and 1c were similar in their opiate activity in vivo. Using the optical isomers of cis-3-methylfentanyl as reference compounds, we analyzed the effects on the pharmacological activities of introducing a phenylethyl 2-hydroxyl group into the molecule.(ABSTRACT TRUNCATED AT 400 WORDS)
(±)-顺式-N-[1-(2-羟基-2-苯乙基)-3-甲基-4-哌啶基]-N-苯基丙酰胺(1)是四种立体异构体[(2S,3R,4S)-1a、(2R,3R,4S)-1b、(2R,3S,4R)-1c和(2S,3S,4R)-1d]的混合物,它们共同构成两对非对映异构的旋光异构体。这四种立体异构体由已知绝对构型的旋光活性中间体通过对哌啶3-位和4-位碳构型无影响的方法制备。通过对(2S,3S,4R)-1d进行X射线分析确定了最终产物中苯乙基2-位碳的构型。将最终产物与奥芬太尼进行1H NMR比较,确定先前称为奥芬太尼的外消旋对是(2S,3R,4S)-1a和(2R,3S,4R)-1c的混合物。在各种结合和药理学试验中评估了1a、1b、1c和1d的个体活性。结合数据表明,异构体1b和1c对用[3H]DAMGO标记的μ位点具有最高的亲和力和选择性。相比之下,四种异构体置换[3H]埃托啡的顺序为1a≈1b>>1c≈1d。在小鼠输精管(MVD)制备物上对这四种异构体的评估显示效价顺序为1a>1b>1c>1d,1a和1b的浓度在飞摩尔范围内即可引起抑制。使用拮抗剂纳曲酮(μ)、ICI 174864(δ)和去甲二氢吗啡酮(κ)进行的实验表明,1a的作用主要由μ受体介导,而δ和κ激动剂作用均参与了1b和1c的作用。异构体1d在MVD制备物中作为一种弱μ拮抗剂起作用。在小鼠镇痛试验和恒河猴单剂量抑制研究中观察到相同的效价顺序。从后一项研究中估计,1a的效价是吗啡的20000-50000倍,使该异构体成为已知最强效的阿片类药物之一。在恒河猴研究中,异构体1d不能替代吗啡,并且在0.6、3.0和6.0mg/kg剂量下似乎会加剧戒断反应。根据小鼠数据,异构体1a的效力比1d高21000倍,而异构体1b和1c在体内的阿片类活性相似。以顺式-3-甲基芬太尼的旋光异构体作为参考化合物,我们分析了在分子中引入苯乙基2-羟基对药理活性的影响。(摘要截取自400字)
