Fleminger S, Rupniak N M, Hall M D, Jenner P, Marsden C D
Biochem Pharmacol. 1983 Oct 1;32(19):2921-7. doi: 10.1016/0006-2952(83)90397-0.
Administration of haloperidol (5 mg/kg i.p.), cis-flupenthixol (2.5 mg/kg i.p.) or sulpiride (2 X 100 mg/kg i.p.) daily for 21 days followed by a 3-day drug withdrawal period caused equivalent cerebral dopamine receptor supersensitivity as judged by enhanced apomorphine-induced stereotypy. These treatments also produced equivalent rises in the number of adenylate cyclase-independent dopamine receptors (D-2) in both striatal and mesolimbic tissue as assessed by specific [3H]spiperone and [3H]N,n-propylnorapomorphine (NPA) binding. No change in the dissociation constant (KD) was apparent in response to neuroleptic treatment. However, only repeated administration of cis-flupenthixol caused an increase in the number of adenylate cyclase-linked dopamine receptors (D-1) in striatum as assessed by enhanced [3H]piflutixol binding and increased dopamine-stimulated cyclic AMP formation. The dissociation constant for [3H]piflutixol binding was unchanged by cis-flupenthixol administration. No change in D-1 receptor numbers or dopamine stimulation of adenylate cyclase occurred in mesolimbic tissue. Repeated treatment with sulpiride or haloperidol was without effect on either [3H]piflutixol binding to D-1 receptors or cyclic AMP formation. In conclusion, increased apomorphine-induced stereotypy following subacute neuroleptic treatment correlates with changes in D-2 receptor numbers, but not with changes in D-1 receptors.
每天腹腔注射氟哌啶醇(5毫克/千克)、顺式氟奋乃静(2.5毫克/千克)或舒必利(2×100毫克/千克),持续21天,随后停药3天,结果显示,根据阿扑吗啡诱导的刻板行为增强判断,三者引起的脑多巴胺受体超敏反应相当。通过特异性的[3H]螺哌隆和[3H]N,N-丙基去甲阿扑吗啡(NPA)结合实验评估,这些处理还使纹状体和中脑边缘组织中不依赖腺苷酸环化酶的多巴胺受体(D-2)数量等量增加。抗精神病药物治疗后,解离常数(KD)没有明显变化。然而,只有反复注射顺式氟奋乃静会使纹状体中与腺苷酸环化酶相连的多巴胺受体(D-1)数量增加,这是通过增强的[3H]匹氟噻醇结合实验以及多巴胺刺激的环磷酸腺苷生成增加来评估的。顺式氟奋乃静给药后,[3H]匹氟噻醇结合的解离常数没有改变。中脑边缘组织中的D-1受体数量或多巴胺对腺苷酸环化酶的刺激均未发生变化。反复使用舒必利或氟哌啶醇治疗对[3H]匹氟噻醇与D-1受体的结合或环磷酸腺苷生成均无影响。总之,亚急性抗精神病药物治疗后阿扑吗啡诱导的刻板行为增强与D-2受体数量的变化相关,而与D-1受体的变化无关。
