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1-羟基-3-氨基吡咯烷-2(HA-966):一种新型γ-氨基丁酸样化合物,在锥体外系疾病中具有潜在应用价值。

1-Hydroxy-3-amino-pyrrolidone-2(HA-966): a new GABA-like compound, with potential use in extrapyramidal diseases.

作者信息

Bonta I L, De Vos C J, Grijsen H, Hillen F C, Noach E L, Sim A W

出版信息

Br J Pharmacol. 1971 Nov;43(3):514-35. doi: 10.1111/j.1476-5381.1971.tb07182.x.

DOI:10.1111/j.1476-5381.1971.tb07182.x
PMID:5157720
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1665789/
Abstract
  1. The drug HA-966 (1-hydroxy-3-amino-pyrrolidone-2), which chemically resembles the cyclic form of GABA, has been studied for neuro-pharmacological properties and for effects on the catecholamine content of the corpus striatum.2. The acute effects on spontaneous behaviour of rodents included flaccid catalepsy and reversible tranquillization in doses which were 5% or less of the lethal dose. Long lasting depression of the CNS, followed by complete recovery, was produced in the cat and the dog. In the monkey HA-966 caused periodical sleeping episodes.3. The exploratory behaviour and the amphetamine-induced motor activity in mice were blocked by HA-966. The toxicity of amphetamine in aggregated mice was only moderately reduced, suggesting that HA-966 differs from neuroleptics.4. Tremors induced by chemical agents (nicotine, zinc and tremorine) were markedly inhibited by HA-966. The muscarinic effects of tremorine were not reduced by HA-966, indicating a selective central antitremor effect.5. HA-966 elevated the threshold to strychnine convulsions and abolished the ipsilateral flexor reflex, while not having motor endplate blocking properties. It is suggested that HA-966 depresses central internuncial neurones.6. In rats and rabbits HA-966 produced synchronous EEG and inhibited the sensory arousal in doses not causing sedation. In the monkey the drug caused a periodical dissociation between ;sleep-EEG' and behaviour.7. In rat brain, HA-966 selectively elevated the dopamine content in the corpus striatum, while no changes in noradrenaline and 5-hydroxytryptamine contents could be demonstrated. The effect was still present when dopa synthesis was inhibited with alpha-methyl-p-tyrosine.8. Several effects of intravenously administered HA-966 became manifest after an appreciable delay and in hepatectomized mice the effects were much reduced. It is postulated that HA-966 is converted to a pharmacologically active metabolite.9. The results are discussed in the light of current views on drug therapy in extrapyramidal conditions and a GABA-related hypothesis as to the mode of action of HA-966 is presented.
摘要
  1. 药物HA - 966(1 - 羟基 - 3 - 氨基 - 吡咯烷酮 - 2),其化学结构类似于GABA的环状形式,已针对其神经药理学特性以及对纹状体中儿茶酚胺含量的影响进行了研究。

  2. 对啮齿动物自发行为的急性影响包括在剂量为致死剂量的5%或更低时出现松弛性僵住症和可逆性镇静作用。猫和狗会出现中枢神经系统的长期抑制,随后完全恢复。在猴子身上,HA - 966会导致周期性睡眠发作。

  3. HA - 966可阻断小鼠的探究行为和苯丙胺诱导的运动活动。HA - 966仅适度降低了聚集小鼠中苯丙胺的毒性,这表明HA - 966与抗精神病药物不同。

  4. HA - 966可显著抑制化学试剂(尼古丁、锌和震颤素)诱导的震颤。HA - 966并未降低震颤素的毒蕈碱样作用,表明其具有选择性的中枢抗震颤作用。

  5. HA - 966提高了对士的宁惊厥的阈值,并消除了同侧屈肌反射,同时不具有运动终板阻断特性。有人认为HA - 966可抑制中枢中间神经元。

  6. 在大鼠和兔子中,HA - 966可产生同步脑电图,并在不引起镇静的剂量下抑制感觉唤醒。在猴子身上,该药物会导致“睡眠脑电图”与行为之间的周期性分离。

  7. 在大鼠脑中,HA - 966可选择性提高纹状体中的多巴胺含量,而未发现去甲肾上腺素和5 - 羟色胺含量有变化。在用α - 甲基 - p - 酪氨酸抑制多巴合成时,这种作用仍然存在。

  8. 静脉注射HA - 966的几种作用在明显延迟后才显现出来,并且在肝切除的小鼠中这些作用大大减弱。据推测,HA - 966会转化为一种具有药理活性的代谢产物。

  9. 根据目前关于锥体外系疾病药物治疗的观点对结果进行了讨论,并提出了一个关于HA - 966作用方式的与GABA相关的假说。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3bf/1665789/b7adceab931b/brjpharm00491-0052-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3bf/1665789/c6aec3c3a61a/brjpharm00491-0046-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3bf/1665789/b7adceab931b/brjpharm00491-0052-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3bf/1665789/c6aec3c3a61a/brjpharm00491-0046-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3bf/1665789/b7adceab931b/brjpharm00491-0052-a.jpg

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