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在红藻氨酸盐癫痫模型中,大鼠海马体中NMDAR1剪接变体的持久增强表达。

Long-lasting enhanced expression in the rat hippocampus of NMDAR1 splice variants in a kainate model of epilepsy.

作者信息

Rafiki A, Ben-Ari Y, Khrestchatisky M, Represa A

机构信息

Université René Descartes (Paris V), France.

出版信息

Eur J Neurosci. 1998 Feb;10(2):497-507. doi: 10.1046/j.1460-9568.1998.00054.x.

DOI:10.1046/j.1460-9568.1998.00054.x
PMID:9749712
Abstract

Chronic epilepsy is associated with increased excitability which may result from abnormal glutamatergic synaptic transmission involving altered properties of N-methyl-D-aspartate (NMDA) receptors. To date two gene families encoding NMDA receptor subunits have been cloned, NR1 and NR2. Eight NR1 mRNAs are generated by alternative splicing of exons 5, 21 and 22; the NR1-1 to NR1-4 C-terminal variants exist in the a or b version depending on the presence or absence of the domain encoded by exon 5. Epilepsy was induced in rats by unilateral intra-amygdalar injection of kainate and animals were killed from 6 h to 4 months following the injection. Increased NR1 mRNA levels were observed during status epilepticus (6-24 h after the injection), both psilateral and contralateral, while a second wave of NMDAR1 mRNA increase occurred in chronic epileptic animals, between 21 days and 4 months following kainate injection. Our data show: (i) a permanent increase of the NR1-2a and NR1-2b mRNA species (containing exon 22) in all hippocampal fields, both ipsilateral and contralateral, and (ii) an increase of the NR1-3 (a and b) mRNAs (containing exon 21) in the ipsilateral CA1, and NR1-3a mRNA in the ipsilateral dentate gyrus. No long-term changes were observed for the NR1-1 and NR14 splice variants. In the ipsilateral CA3 area a globally decreased mRNA expression was associated with neuronal loss. A possible contribution to the maintenance of the epileptic state by an increased expression of NMDA receptors is discussed.

摘要

慢性癫痫与兴奋性增加有关,这可能是由于涉及N-甲基-D-天冬氨酸(NMDA)受体特性改变的异常谷氨酸能突触传递所致。迄今为止,已克隆出两个编码NMDA受体亚基的基因家族,即NR1和NR2。通过外显子5、21和22的可变剪接产生8种NR1 mRNA;NR1-1至NR1-4 C末端变体根据外显子5编码的结构域的存在与否以α或β版本存在。通过单侧杏仁核内注射海藻酸在大鼠中诱发癫痫,并在注射后6小时至4个月处死动物。在癫痫持续状态期间(注射后6 - 24小时),同侧和对侧均观察到NR1 mRNA水平升高,而在慢性癫痫动物中,即在海藻酸注射后21天至4个月之间,出现了第二轮NMDAR1 mRNA增加。我们的数据显示:(i)同侧和对侧所有海马区中NR1-2a和NR1-2b mRNA种类(包含外显子22)持续增加,以及(ii)同侧CA1区中NR1-3(α和β)mRNA(包含外显子21)增加,同侧齿状回中NR1-3a mRNA增加。未观察到NR1-1和NR1-4剪接变体的长期变化。在同侧CA3区,整体mRNA表达下降与神经元丢失有关。文中讨论了NMDA受体表达增加对癫痫状态维持的可能作用。

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