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论新合成多巴胺在纹状体功能中的主要作用。

On a prime role for newly synthesized dopamine in striatal function.

作者信息

Shore P A, Dorris R L

出版信息

Eur J Pharmacol. 1975 Feb;30(2):315-8. doi: 10.1016/0014-2999(75)90115-6.

Abstract

Rats were given either the tyrosine hydroxylase inhibitor, alpha-methyltyrosine (alphaMT), in doses of 10 or 250 mg/kg or the neuroleptic, haloperidol (0.25 mg/kg). Other rats received both drugs (haloperidol 30 min after alphaMT). This dose of haloperidol alone caused only a slight, gradually developing catalepsy, while alphaMT alone caused none. The combination quickly caused a strong catalepsy. Striatal dopamine (DA) stores were only minimally depleted at the time of catalepsy potentiation. Th e marked elevation of striatal homovanilluc acid concentration seen after haloperidol administration was greatly inhibited by alphaMT pretreatment. It is concluded that the marked potentiation of haloperidol-induced catalepsy by alpha MT is related to the absence of newly synthesized DA rather than to an exhausted main DA pool and that newly synthesized DA has a greater role in striatal function than does DA of the main striatal storage pool.

摘要

给大鼠分别注射剂量为10或250毫克/千克的酪氨酸羟化酶抑制剂α-甲基酪氨酸(αMT)或抗精神病药物氟哌啶醇(0.25毫克/千克)。其他大鼠同时接受这两种药物(在注射αMT 30分钟后注射氟哌啶醇)。单独使用该剂量的氟哌啶醇仅引起轻微的、逐渐发展的僵住症,而单独使用αMT则不会引起僵住症。联合用药迅速引起强烈的僵住症。在僵住症增强时,纹状体多巴胺(DA)储备仅轻微减少。αMT预处理极大地抑制了氟哌啶醇给药后纹状体高香草酸浓度的显著升高。得出的结论是,αMT对氟哌啶醇诱导的僵住症的显著增强作用与新合成的DA的缺乏有关,而非与主要DA储备池耗尽有关,并且新合成的DA在纹状体功能中的作用比主要纹状体储存池中的DA更大。

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