SB-236057-A:一种选择性5-HT1B受体逆激动剂。

C. Roberts, J. Watson, Gary W. Price, D. Middlemiss
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引用次数: 17

摘要

5-HT1B自身受体参与控制5-羟色胺能神经元末端和细胞体区域的细胞外5-羟色胺水平。在这篇文章中,我们回顾了选择性和有效的5-HT1B受体逆激动剂SB-236057-A(1'-乙基-5-(2'-甲基-4'-(5-甲基-1,3,4-恶二唑-2-基)联苯-4-羰基)-2,3,6,7-四氢螺(呋喃[2,3-f]吲哚-3,4'-哌啶)盐酸盐)的药理学和药代动力学数据。SB 236057-A已被证明对人类5-HT1B受体具有高亲和力(pK(i) = 8.2),并且对人类5-HT1B受体的选择性比其他5-HT受体和一系列其他受体、离子通道和酶高80倍或更多。在人类5-HT1B受体的功能研究中,SB-236057-A通过[(35)S]GTPgammaS结合表现出反向拮抗作用(pA(2) = 8.9),通过cAMP积累表现出沉默拮抗作用(pA(2) = 9.2)。SB-236057-A还可作为5-HT末端自受体的拮抗剂,通过电刺激豚鼠和人皮层切片的[3H]5-HT释放来测定。在豚鼠体内,药代动力学分析表明SB-236057-A具有生物利用性,体内药效学分析表明SB-236057-A可进入大脑并具有较长的作用时间。重要的是,在相关剂量下,从焦虑、心血管、镇静或偏头痛的角度来看,没有明显的副作用。体内微透析研究表明,SB-236057-A在豚鼠皮层中是一种拮抗剂,但对细胞外5-HT水平本身没有影响。相反,SB-236057-A增加了豚鼠齿状回细胞外5-HT水平。这种5-HT释放的增加与给予帕罗西汀14天后观察到的相同。SB-236057-A一直是确认豚鼠或人类末端5-HT自身受体为5-HT1B亚型的有用工具。似乎急性5-HT1B受体阻断,通过增加齿状回中5-HT的释放,可能提供一种快速作用的抗抑郁药。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
SB-236057-A: a selective 5-HT1B receptor inverse agonist.
5-HT1B autoreceptors are involved in the control of extracellular 5-HT levels from both the terminal and cell body regions of serotonergic neurons. In this manuscript we review the pharmacological and pharmacokinetic data available for the selective and potent 5-HT1B receptor inverse agonist, SB-236057-A (1'-ethyl-5-(2'-methyl-4'-(5-methyl-1,3,4-oxadiazolyl-2-yl)biphenyl-4-carbonyl)-2,3,6,7-tetrahydrospiro (furo[2,3-f]indole-3,4'-piperidine) hydrochloride). SB 236057-A has been shown to have high affinity for human 5-HT1B receptors (pK(i) = 8.2) and displays 80 or more fold selectivity for the human 5-HT1B receptor over other 5-HT receptors and a range of additional receptors, ion channels and enzymes. In functional studies at human 5-HT1B receptors SB-236057-A displayed inverse agonism (pA(2) = 8.9) using [(35)S]GTPgammaS binding, and silent antagonism (pA(2) = 9.2) using cAMP accumulation. SB-236057-A also acted as an antagonist at the 5-HT terminal autoreceptor as measured by [3H]5-HT release from electrically stimulated guinea pig and human cortical slices. In the guinea pig, pharmacokinetic analysis demonstrated that SB-236057-A was bioavailable and according to in vivo pharmacodynamic assays it enters brain and has a long duration of action. Importantly no side effect liability was evident at relevant doses from anxiogenic, cardiovascular, sedative or migraine viewpoints. In vivo microdialysis studies demonstrated that SB-236057-A is an antagonist in the guinea pig cortex but has no effect on extracellular 5-HT levels per se. In contrast, SB-236057-A increased extracellular 5-HT levels in the guinea pig dentate gyrus. This increase in 5-HT release was comparable to that observed after 14 days of paroxetine administration. SB-236057-A has been a useful tool in confirming that, in either guinea pigs or humans, the terminal 5-HT autoreceptor is of the 5-HT1B subtype. It appears that acute 5-HT1B receptor blockade, by virtue of increased 5-HT release in the dentate gyrus, may provide a rapidly acting antidepressant.
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