首页> 外文期刊>The European Journal of Neuroscience >Gene expression analysis of the emergence of epileptiform activity after focal injection of kainic acid into mouse hippocampus.
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Gene expression analysis of the emergence of epileptiform activity after focal injection of kainic acid into mouse hippocampus.

机译:小鼠海马体局部注入海藻酸后,癫痫样活动出现的基因表达分析。

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We report gene profiling data on genomic processes underlying the progression towards recurrent seizures after injection of kainic acid (KA) into the mouse hippocampus. Focal injection enabled us to separate the effects of proepileptic stimuli initiated by KA injection. Both the injected and contralateral hippocampus participated in the status epilepticus. However, neuronal death induced by KA treatment was restricted to the injected hippocampus, although there was some contralateral axonal degeneration. We profiled gene expression changes in dorsal and ventral regions of both the injected and contralateral hippocampus. Changes were detected in the expression of 1526 transcripts in samples from three time-points: (i) during the KA-induced status epilepticus, (ii) at 2 weeks, before recurrent seizures emerged, and (iii) at 6 months after seizures emerged. Grouping genes with similar spatio-temporal changes revealed an early transcriptional response, strong immune, cell death and growth responses at 2 weeks and an activation of immune and extracellular matrix genes persisting at 6 months. Immunostaining for proteins coded by genes identified from array studies provided evidence for gliogenesis and suggested that the proteoglycan biglycan is synthesized by astrocytes and contributes to a glial scar. Gene changes at 6 months after KA injection were largely restricted to tissue from the injection site. This suggests that either recurrent seizures might depend on maintained processes including immune responses and changes in extracellular matrix proteins near the injection site or alternatively might result from processes, such as growth, distant from the injection site and terminated while seizures are maintained.
机译:我们报告基因分析过程的基础上向海藻酸(KA)注射海藻酸(KA)注射后向复发性癫痫发作的进展的基因组过程数据。局部注射使我们能够区分由KA注射引发的癫痫刺激的作用。注射的海马和对侧海马都参与了癫痫持续状态。然而,尽管存在一些对侧轴突变性,但由KA治疗诱导的神经元死亡仅限于注射的海马。我们分析了注射和对侧海马的背侧和腹侧区域的基因表达变化。从三个时间点检测到样本中1526个转录物的表达发生了变化:(i)在KA诱发的癫痫持续状态中,(ii)在复发发作前2周,以及(iii)发作后6个月。将具有相似时空变化的基因分组显示在2周时早期转录反应,强烈的免疫,细胞死亡和生长反应,并在6个月时持续存在免疫和细胞外基质基因的激活。对通过阵列研究鉴定的基因编码的蛋白质进行的免疫染色提供了胶质发生的证据,并表明蛋白聚糖双糖链蛋白聚糖是由星形胶质细胞合成的,并导致神经胶质瘢痕。 KA注射后6个月的基因变化主要局限于注射部位的组织。这表明,复发性癫痫发作可能取决于维持的过程,包括免疫应答和注射部位附近细胞外基质蛋白的变化,或者可能是由诸如生长,远离注射部位并在维持癫痫发作时终止的过程引起的。

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