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Glutamate Uptake into Synaptic Vesicles: Competitive Inhibition by Bromocriptine

机译:谷氨酸摄入突触囊泡:溴隐亭的竞争抑制作用

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摘要

The ATP-dependent uptake of l-glutamate into synaptic vesicles has been well characterized, implicating a key role for synaptic vesicles in glutamatergic neurotransmission. In the present study, we provide evidence that vesicular glutamate uptake is selectively inhibited by the pep-tide-containing halogenated ergot bromocriptine. It is the most potent inhibitor of the agents tested; the IC 5 o was de-termined to be 22 Μ M . The uptake was also inhibited by other ergopeptines such as ergotamine and ergocristine, but with less potency. Ergots devoid of the peptide moiety, however, such as ergonovine, lergotrile, and methysergide, had little or no effect. Although bromocriptine is known to elicit dopaminergic and serotonergic effects, its inhibitory effect on vesicular glutamate uptake was not mimicked by agents known to interact with dopamine and serotonin receptors. Kinetic data suggest that bromocriptine competes with glutamate for the glutamate binding site on the glutamate trans-locator. It is proposed that this inhibitor could be useful as a prototype probe in identifying and characterizing the vesicular glutamate translocator, as well as in developing a more specific inhibitor of the transport system.
机译:L-谷氨酸的ATP依赖性摄取到突触囊泡的特征在于,表征了很好的表征,对谷氨酸神经递质中的突触囊泡表示关键作用。在本研究中,我们提供了含有含孔的卤化耳廓溴隐亭选择性抑制囊泡谷氨酸摄取的证据。它是测试的药剂最有效的抑制剂; IC 5 O被解除为22μm。其他ergopeptines如奥替胺和迈尔格氏菌素的摄取也抑制了摄取,但效力较小。然而,遗传学缺乏肽部分,例如尔格诺藤,乳酰胺和素合物,几乎没有任何影响。虽然已知溴杉裂引起多巴胺能和血清酰基能效应,但其对囊泡谷氨酸摄取的抑制作用未被已知与多巴胺和血清素受体相互作用的试剂。动力学数据表明,溴杉木与谷氨酸反式定位器上的谷氨酸结合位点的谷氨酸竞争。提出,该抑制剂可用作鉴定和表征囊泡谷氨酸偶偶联剂的原型探针,以及开发更具体的运输系统的抑制剂。

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