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自受体介导的γ-氨基丁酸释放调节:摄取抑制的作用及新型γ-氨基丁酸B受体拮抗剂的影响

Autoreceptor-mediated regulation of GABA release: role of uptake inhibition and effects of novel GABAB antagonists.

作者信息

Waldmeier P C, Hertz C, Wicki P, Grunenwald C, Baumann P A

机构信息

Research Department, Ciba-Geigy AG, Basel, Switzerland.

出版信息

Naunyn Schmiedebergs Arch Pharmacol. 1993 May;347(5):514-20. doi: 10.1007/BF00166744.

DOI:10.1007/BF00166744
PMID:8391653
Abstract

While the role of GABAB autoreceptors in the regulation of GABA release in synaptosomes and brain slices is well established, little is known about their role in vivo. Doubts have arisen because there is an apparent discrepancy between the frequencies at which GABA neurons fire and the frequency range within which autoreceptor regulation is observed in vitro. To see whether this apparent mismatch could be due to the use of a GABA uptake inhibitor in the release experiments in slices, we have compared the frequency dependencies of GABA release in the presence and absence of uptake inhibition. Before-hand, the previously incomplete frequency curve in the presence of uptake inhibition was extended at the lower end. To achieve this, stimulation was performed by means of groups of 4 pseudo-one-pulses (POP's) at inter-POP intervals corresponding to frequencies of 0.015625-0.5 Hz. It could be shown that activation of the GABAB autoreceptor by endogenously released GABA begins at a stimulation frequency as low as 0.0625 Hz. Experiments with the antagonist, CGP 35348, at inter-POP intervals of 1 min, at which the preceding POP has no longer an effect on GABA release during the next one, showed that basal release alone already substantially activated the autoreceptor. The frequency dependence in the absence as compared to the presence of uptake inhibition was shifted towards higher frequencies by a factor of 4. We do not consider this enough to remove our doubts about the in vivo operativity of GABAB autoreceptors.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

虽然GABAB自身受体在调节突触体和脑片中GABA释放方面的作用已得到充分证实,但对其在体内的作用却知之甚少。人们产生了疑问,因为GABA神经元的放电频率与体外观察到的自身受体调节频率范围之间存在明显差异。为了探究这种明显的不匹配是否可能是由于在脑片释放实验中使用了GABA摄取抑制剂,我们比较了存在和不存在摄取抑制时GABA释放的频率依赖性。事先,在存在摄取抑制的情况下先前不完整的频率曲线在下端得到了扩展。为此,通过以对应于0.015625 - 0.5 Hz频率的脉冲间间隔进行4个伪单脉冲(POP)组刺激。结果表明,内源性释放的GABA对GABAB自身受体的激活始于低至0.0625 Hz的刺激频率。在脉冲间间隔为1分钟时使用拮抗剂CGP 35348进行的实验表明,在此间隔下前一个POP在下一个POP期间对GABA释放不再有影响,这表明仅基础释放就已充分激活了自身受体。与存在摄取抑制相比,不存在摄取抑制时的频率依赖性向更高频率偏移了4倍。我们认为这不足以消除我们对GABAB自身受体在体内可操作性的疑虑。(摘要截断于250字)

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GABA release in rat cortical slices is unable to cope with demand if the autoreceptor is blocked.如果自身受体被阻断,大鼠皮层切片中的γ-氨基丁酸释放将无法满足需求。
Naunyn Schmiedebergs Arch Pharmacol. 1994 Jun;349(6):583-7. doi: 10.1007/BF01258463.
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GABA and glutamate release affected by GABAB receptor antagonists with similar potency: no evidence for pharmacologically different presynaptic receptors.GABAB受体拮抗剂以相似效力影响GABA和谷氨酸释放:无药理学上不同的突触前受体的证据。
Br J Pharmacol. 1994 Dec;113(4):1515-21. doi: 10.1111/j.1476-5381.1994.tb17168.x.
Evidence against a functional link between noradrenaline uptake mechanisms and presynaptic alpha-2 adrenoceptors.反对去甲肾上腺素摄取机制与突触前α-2肾上腺素能受体之间存在功能联系的证据。
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Species differences in presynaptic serotonin autoreceptors: mainly 5-HT1B but possibly in addition 5-HT1D in the rat, 5-HT1D in the rabbit and guinea-pig brain cortex.突触前5-羟色胺自身受体的种属差异:在大鼠中主要为5-HT1B,可能还包括5-HT1D;在兔和豚鼠脑皮层中为5-HT1D。
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