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首页> 外文OA文献 >Pharmacological activities of optically pure enantiomers of the κ opioid agonist, U50,488, and its cis diastereomer: evidence for three κ receptor subtypes
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Pharmacological activities of optically pure enantiomers of the κ opioid agonist, U50,488, and its cis diastereomer: evidence for three κ receptor subtypes

机译:κAphioid激动剂,U50,488及其顺式非对映异构体的光学纯对映体的药理活性:三种κ受体亚型的证据

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De Costa et al. (FEBS Lett. 223, 335; 1987) recently described the synthesis of optically pure enantiomers of (+/-)-trans-3,4-dichloro-N-methyl-N-[2-(1-pyrrolidinyl)-cyclohexyl]benzeneacetamide (U50,488). In the present study we examined the in vitro opioid receptor selectivity of (-)-(1S,2S)-U50,488, (+)-(1R,2R)-U50,488 and (+/-)-cis-3,4-di-chloro-N-methyl-N-[2-(1-pyrrolidinyl)-cyclohexyl]benzeneacetamide (the cis diasteromers of U50,488), as well as their pharmacological activities in rhesus monkeys. Using [3H]5[alpha],7[alpha],8[beta]-(-)-N-methyl-N-[7-1-pyrrolidinyl)-1-oxaspiro (4,5)dec-8-yl]-phenyl-benzeneacetamide([3H]U69,593) to label [kappa] binding sites of guinea pig membranes, the apparent dissociation constants of the enantiomers hadU50,488 were 0.89 and 299 nM, for the (S,S) and (R,R) enantiomers, respectively. The (-)-cis and (+)-cis diastereomers had apparent Kds of 167 and 2715 nM, respectively. Binding surface analysis of the interaction of (-)-(1S,2S)-U50,488 with [kappa] binding sites labeled by [3H]bremazocine resolved two binding sites at which (-)-(1S,2S)-U50,488 had Kds of 30 and 10485 nM, respectively. The (+/-)-cis, (-)-cis and (+)-cis diastereomers of U50,488 (1 [mu]M) did not inhibit [3H]bremazocine binding. Rhesus monkeys were trained to discriminate ethylketocyclazocine (EKC) and saline. All compounds tested substituted completely for EKC. The order of potency was (-)-(1S,2S)-U50,488 (+/-)-U50,488 (+/-)-cisdiastereomer of U50,488 (+)-(1R,2R)-U50,488. In tests of analgesia, (-)-(1S,2S)-U50,488 was 2-4 times more potent than (+/-)-U50,488, while (+/-)-cis diastereomer of U50,488 and (+)-(1R,2R)-U50,488 were inactive at the highest doses tested (32 mg/kg). Taken collectively, these data indicate that the pharmacologically active enantiomer of U50,488 is (-)-(1S,2S)-U50,488, and provide preliminary evidence for three subtypes of [kappa] binding sites in guinea pig brain.
机译:德科斯塔等人。 (FEBS快报223,335; 1987)最近描述的(+/-)光学纯的对映体的合成 - 反式-3,4-二氯-N-甲基-N- [2-(1-吡咯烷基)环己基]苯乙酰胺(U50,488)。在本研究中,我们检测了在体外阿片样受体的选择性( - ) - (1S,2S)-U50,488,(+) - (1R,2R)-U50,488和(+/-) - 顺-3-三2,4-二氯代-N-甲基-N- [2-(1-吡咯烷基)环己基]苯乙酰胺(U50,488的非对映体顺式),以及在猕猴中其药理活性。使用[3H] 5α,7α,8-β - ( - ) - N-甲基-N- [7-1吡咯烷基)-1-氧杂螺(4,5)癸-8-基] - 苯基 - 苯乙酰胺([3 H] U69,593)至标签κ-结合豚鼠膜的位点,对映异构体的表观解离常数hadU50,488为0.89和299 nM的,对于(S,S)和( R,R)对映体,分别。的( - ) - 顺式和(+) - 顺式非对映体分别具有167和2715纳米的表观的Kd。 ( - ) - 的相互作用的结合表面分析(1S,2S)与-U50,488κ-结合通过[3 H]布马佐辛解决两个结合位点在该标记位点( - ) - (1S,2S)-U50, 488分别具有30和10485纳米的Kd。的(+/-) - 顺式,( - ) - 顺式和(+) - 顺式U50,488的非对映体(1微摩尔)不抑制[3 H]结合布马佐辛。恒河猴进行了培训,以判别ethylketocyclazocine(EKC)和生理盐水。所有化合物测试EKC完全地取代。效力的次序为( - ) - (1S,2S)-U50,488>(+/-) - U50,488>(+/-) - U50,488的cisdiastereomer>(+) - (1R,2R) -U50,488。镇痛试验中,( - ) - (1S,2S)-U50,488是2-4倍更有效的(+/-) - U50,488,而(+/-) - 顺式U50,488和非对映体(+) - (1R,2R)-U50,488无活性在最高剂量测试(32毫克/千克)。采取集体,这些数据表明,U50,488的药理活性的对映体是( - ) - (1S,2S)-U50,488,和豚鼠大脑κ-结合位点的三种亚型提供的初步证据。

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