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溴隐亭(CB 154)对“调节性”多巴胺受体进行选择性和长效刺激的证据。

Evidence for selective and long-lasting stimulation of "regulatory" dopamine-receptors by bromocriptine (CB 154).

作者信息

di Chiara G, Porceddu M L, Vargiu L, Stefanini E, Gessa G L

出版信息

Naunyn Schmiedebergs Arch Pharmacol. 1977 Nov;300(3):239-45. doi: 10.1007/BF00500966.

Abstract

Bromocriptine, an ergot-derivate with DA-receptor stimulating properties in vivo, produces long-lasting hypomotility in mice not accustomed to the motility cage and decreases brain DOPAC and HVA without affecting brain DA. These effects are obtained with doses 25 times lower than those which produce hypermotility. The decrease of brain DOPAC is correlated to the hypomotility both on a dose- and on a time-basis. Potent neuroleptics as pimozide, benzperidol and droperidol, which are considered to be fairly specific DA-receptor blockers, antagonize the hypomotility and the decrease of brain DOPAC produced by bromocriptine. These effects are obtained with very low doses (0.05--0.3 mg/kg) of neuroleptics which per se do not affect motility or brain DOPAC. The maximal decrease of brain DOPAC and HVA produced by bromocriptine is similar to that produced by apomorphine and the combination of these drugs does not result in a further decrease of brain DOPAC or HVA. On the basis of these results it is postulated that bromocriptine decreases brain DA-turnover and produces hypomotility by acting on "regulatory" DA-receptors different from the post-synaptic ones of the "terminal" dopaminergic areas.

摘要

溴隐亭是一种在体内具有刺激多巴胺(DA)受体特性的麦角衍生物,它能使不习惯活动笼的小鼠产生持久的运动减少,并降低脑内3,4-二羟基苯乙酸(DOPAC)和高香草酸(HVA)的水平,而不影响脑内多巴胺(DA)的含量。产生这些效应所需的剂量比引起运动亢进的剂量低25倍。脑内DOPAC的降低在剂量和时间上都与运动减少相关。强效抗精神病药物如匹莫齐特、苄哌利多和氟哌利多,被认为是相当特异的DA受体阻滞剂,它们能拮抗溴隐亭引起的运动减少和脑内DOPAC的降低。这些效应是在非常低剂量(0.05 - 0.3毫克/千克)的抗精神病药物作用下产生的,而这些药物本身并不影响运动或脑内DOPAC。溴隐亭引起的脑内DOPAC和HVA的最大降低程度与阿扑吗啡引起的相似,并且这两种药物联合使用不会导致脑内DOPAC或HVA的进一步降低。基于这些结果,推测溴隐亭通过作用于不同于“终末”多巴胺能区域突触后受体的“调节性”DA受体,降低脑内DA的周转率并产生运动减少。

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