SCH 23390对配体与小牛纹状体多巴胺D1受体结合的优先抑制作用。
Preferential inhibition of ligand binding to calf striatal dopamine D1 receptors by SCH 23390.
作者信息
Cross A J, Mashal R D, Johnson J A, Owen F
出版信息
Neuropharmacology. 1983 Nov;22(11):1327-9. doi: 10.1016/0028-3908(83)90208-3.
PMID:6141534
Abstract
The phenylbenzazepine derivative, SCH 23390 was found to be a potent inhibitor of 3H-piflutixol binding to calf striatal dopamine D1 receptors. In contrast SCH 23390 was only a weak inhibitor of 3H-spiperone binding to dopamine D2 receptors. Although possessing some activity at serotonin S2 and alpha 2 adrenergic receptors, SCH 23390 appears to be a potent and selective D1 receptor antagonist.
摘要
苯基苯并氮杂卓衍生物SCH 23390被发现是3H-匹氟噻吨与小牛纹状体多巴胺D1受体结合的强效抑制剂。相比之下,SCH 23390只是3H-螺哌隆与多巴胺D2受体结合的弱抑制剂。尽管SCH 23390在5-羟色胺S2和α2肾上腺素能受体上具有一定活性,但它似乎是一种强效且选择性的D1受体拮抗剂。
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