Street Leslie J, Sternfeld Francine, Jelley Richard A, Reeve Austin J, Carling Robert W, Moore Kevin W, McKernan Ruth M, Sohal Bindi, Cook Susan, Pike Andrew, Dawson Gerard R, Bromidge Frances A, Wafford Keith A, Seabrook Guy R, Thompson Sally A, Marshall George, Pillai Goplan V, Castro José L, Atack John R, MacLeod Angus M
Departments of Medicinal Chemistry, Biochemistry, and Pharmacology, Merck Sharp and Dohme Research Laboratories, Neuroscience Research Centre, Terlings Park, Eastwick Road, Harlow, Essex CM20 2QR, UK.
J Med Chem. 2004 Jul 1;47(14):3642-57. doi: 10.1021/jm0407613.
The identification of a novel series of 7,8,9,10-tetrahydro-(7,10-ethano)-1,2,4-triazolo[3,4-a]phthalazines as GABA(A)alpha5 inverse agonists, which have both binding and functional (efficacy) selectivity for the benzodiazepine binding site of alpha5- over alpha1-, alpha2-, and alpha3-containing GABA(A) receptor subtypes, is described. Binding selectivity was determined to a large part by the degree of planarity of the fused ring system whereas functional selectivity was dependent on the nature of the heterocycle at the 3-position of the triazolopyridazine ring. 3-Furan and 5-methylisoxazole were shown to be optimal for GABA(A)alpha5 functional selectvity. 3-(5-Methylisoxazol-3-yl)-6-(2-pyridyl)methyloxy-1,2,4-triazolo[3,4-a]phthalazine (43) was identified as a full inverse agonist at the GABA(A)alpha5 subtype with functional selectivity over the other GABA(A) receptor subtypes and good oral bioavailability.
本文描述了一系列新型的7,8,9,10-四氢-(7,10-亚乙基)-1,2,4-三唑并[3,4-a]酞嗪类化合物作为GABA(A)α5反向激动剂,它们对含α5的GABA(A)受体亚型的苯二氮䓬结合位点具有结合和功能(效能)选择性,优于含α1、α2和α3的GABA(A)受体亚型。结合选择性在很大程度上取决于稠环系统的平面度,而功能选择性则取决于三唑并哒嗪环3位杂环的性质。3-呋喃基和5-甲基异恶唑基被证明对GABA(A)α5功能选择性最为理想。3-(5-甲基异恶唑-3-基)-6-(2-吡啶基)甲氧基-1,2,4-三唑并[3,4-a]酞嗪(43)被鉴定为GABA(A)α5亚型的完全反向激动剂,对其他GABA(A)受体亚型具有功能选择性,且口服生物利用度良好。
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