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下丘脑后部注入谷氨酸通过增加海马组胺减少雄性大鼠戊四氮诱发的癫痫发作。

Posterior hypothalamus glutamate infusion decreases pentylenetetrazol-induced seizures of male rats through hippocampal histamine increase.

作者信息

Arzhang Atieh, Elahdadi Salmani Mahmoud, Lashkarbolouki Taghi, Goudarzi Iran

机构信息

Faculty of Biology, Damghan University, Damghan, Iran.

Faculty of Biology, Damghan University, Damghan, Iran.

出版信息

Pharmacol Biochem Behav. 2017 Jul;158:7-13. doi: 10.1016/j.pbb.2017.05.004. Epub 2017 May 8.

DOI:10.1016/j.pbb.2017.05.004
PMID:28495313
Abstract

OBJECTIVES

Seizures are epileptic manifestations that are intrinsically modulated through different neurotransmitters and receptor systems. Although glutamate increases excitation and hence seizures, it activates other systems which could potentially terminate seizures. Histamine originates from neurons of the posterior hypothalamus (PH) and can mediate anticonvulsant properties, but the effect of local PH glutamate on hippocampal histamine content is unknown. Therefore, in this study, the effect of PH glutamate and the involvement of hippocampal histamine in pentylenetetrazol (PTZ) induced seizure activity was studied.

MATERIALS AND METHODS

OX2R antagonist (TCS OX2 29, 40nmol/1μl, intra-PH), AMPA/Kainate receptor antagonist (CNQX, 3mM, intra-PH) and glutamate (1mM) were injected bilaterally into PH using stereotaxic surgery. The intravenous PTZ infusion model was used to generate behavioral convulsions and the amount of hippocampal histamine content was then measured using a biochemical method.

RESULTS

Administration of glutamate into PH decreased both seizure stage and the duration of tonic-clonic convulsion (TCC) with increasing TCC latency and hippocampal histamine content. Blocking OX2Rs alone or coinhibition of OX2Rs and AMPA/kainate receptors reversed these effects by increasing both seizure stage and TCC duration, and by decreasing both latency and consequent histamine content.

CONCLUSIONS

Our findings suggest that glutamate administration into PH may control seizures (stages and duration) through increasing the hippocampal histamine content.

摘要

目的

癫痫发作是通过不同神经递质和受体系统进行内在调节的癫痫表现。虽然谷氨酸会增加兴奋性从而引发癫痫发作,但它也会激活其他可能终止癫痫发作的系统。组胺源自下丘脑后部(PH)的神经元,可介导抗惊厥特性,但局部PH谷氨酸对海马组胺含量的影响尚不清楚。因此,在本研究中,研究了PH谷氨酸的作用以及海马组胺在戊四氮(PTZ)诱导的癫痫活动中的参与情况。

材料与方法

使用立体定向手术将OX2R拮抗剂(TCS OX2 29,40nmol/1μl,双侧PH内注射)、AMPA/海人酸受体拮抗剂(CNQX,3mM,双侧PH内注射)和谷氨酸(1mM)双侧注射到PH中。采用静脉注射PTZ输注模型诱导行为性惊厥,然后使用生化方法测量海马组胺含量。

结果

向PH内注射谷氨酸可降低癫痫发作阶段和强直阵挛性惊厥(TCC)的持续时间,同时增加TCC潜伏期和海马组胺含量。单独阻断OX2Rs或同时抑制OX2Rs和AMPA/海人酸受体会通过增加癫痫发作阶段和TCC持续时间,以及降低潜伏期和随之而来的组胺含量来逆转这些作用。

结论

我们的研究结果表明,向PH内注射谷氨酸可能通过增加海马组胺含量来控制癫痫发作(阶段和持续时间)。

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