Shiosaki K, Jenner P, Asin K E, Britton D R, Lin C W, Michaelides M, Smith L, Bianchi B, Didomenico S, Hodges L, Hong Y, Mahan L, Mikusa J, Miller T, Nikkel A, Stashko M, Witte D, Williams M
Pharmaceutical Products Division, Abbott Laboratories, Abbott Park, Illinois, USA.
J Pharmacol Exp Ther. 1996 Jan;276(1):150-60.
(-)-Trans 9,10-hydroxy-2-propyl-4,5,5a,6,7,11b-hexahydro-3-thia-5- azacyclopent-1-ena[c]phenanthrene hydrochloride (A-86929) is a potent and selective full agonist at the dopamine (DA) D1-like receptor. Judging by its binding affinities to the D1 and D2 classes of receptors, the compound is approximately 20-fold D1 receptor-selective, whereas relative potencies based on functional in vitro assays indicate that A-86929 is greater than 400-fold D1-selective. A-86929 has moderate to weak (Ki > 1 microM) affinity at other monoaminergic and peptidergic receptors, at ion channels and at monoamine uptake sites. The catechol of A-86929 was bis-acetylated to produce the prodrug, (-)-trans 9,10-acetoxy-2-propyl-4,5,5a,6,7,11-b-hexahydro-3-thia- 5-azacyclopent-1-ena[c]phenanthrene hydrochloride (ABT-431), which is more chemically stable yet is rapidly converted to the parent compound with a half-life of less than 1 min in plasma. Both A-86929 and ABT-431 produced contralateral rotation in rats bearing unilateral 6-hydroxydopamine lesions, with ED50 values of 0.24 mumol/kg s.c. and 0.54 mumol/kg s.c., respectively. A-86929 and ABT-431 improved behavioral disability scores and increased locomotor activity in the 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine-lesioned marmoset model of Parkinson's disease in a dose-dependent manner (the minimum effective dose was 0.10 mumol/kg s.c.). When administered three times daily for 30 consecutive days to 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine-lesioned marmosets, A-86929 significantly improved disability scores throughout the duration of the study. Current Parkinson's disease therapy includes L-dopa, which stimulates both classes of DA receptors by virtue of its conversion to DA in vivo, and direct-acting D2-selective agonists. Stimulation of the D2 receptor, which is associated with all current DA agonist-based therapies, may contribute to their dose-limiting side effects. An agent such as A-86929 (or its prodrug ABT-431), which selectively stimulates the D1 receptor, may represent a novel mechanism for Parkinson's disease therapy with the potential for an improved side-effect profile and, consequently, improved patient compliance.
(-)-反式9,10-羟基-2-丙基-4,5,5a,6,7,11b-六氢-3-硫杂-5-氮杂环戊并[1,2-c]菲盐酸盐(A-86929)是一种强效且选择性的多巴胺(DA)D1类受体完全激动剂。从其与D1和D2类受体的结合亲和力判断,该化合物对D1受体的选择性约为20倍,而基于体外功能试验的相对效价表明A-86929对D1受体的选择性大于400倍。A-86929对其他单胺能和肽能受体、离子通道及单胺摄取位点具有中度至弱(Ki>1μM)的亲和力。A-86929的儿茶酚被双乙酰化以产生前药(-)-反式9,10-乙酰氧基-2-丙基-4,5,5a,6,7,11b-六氢-3-硫杂-5-氮杂环戊并[1,2-c]菲盐酸盐(ABT-431),其化学稳定性更高,但在血浆中半衰期小于1分钟时能迅速转化为母体化合物。A-86929和ABT-431在单侧6-羟基多巴胺损伤的大鼠中均产生对侧旋转,ED50值分别为0.24μmol/kg皮下注射和0.54μmol/kg皮下注射。在帕金森病的1-甲基-4-苯基-1,2,3,6-四氢吡啶损伤的狨猴模型中,A-86929和ABT-431以剂量依赖性方式改善行为残疾评分并增加运动活性(最小有效剂量为0.10μmol/kg皮下注射)。当连续30天每天给药3次给1-甲基-4-苯基-1,2,3, ,6-四氢吡啶损伤的狨猴时,A-86929在整个研究期间显著改善残疾评分。目前的帕金森病治疗包括左旋多巴,其通过在体内转化为多巴胺来刺激两类DA受体,以及直接作用的D2选择性激动剂。与目前所有基于DA激动剂的治疗相关联的D2受体刺激可能导致其剂量限制性副作用。像A-86929(或其前药ABT-431)这样选择性刺激D1受体的药物,可能代表一种治疗帕金森病的新机制,具有改善副作用谱的潜力,从而提高患者的依从性。
Zotero 插件