首页> 外文期刊>Journal of Molecular Neuroscience: MN >Expression patterns of miR-124, miR-134, miR-132, and miR-21 in an immature rat model and children with mesial temporal lobe epilepsy
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Expression patterns of miR-124, miR-134, miR-132, and miR-21 in an immature rat model and children with mesial temporal lobe epilepsy

机译:miR-124,miR-134,miR-132和miR-21在未成熟大鼠模型和中颞叶癫痫患儿中的表达模式

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Mesial temporal lobe epilepsy (MTLE) is a particularly devastating form of human epilepsy with significant incidence of medical intractability. MicroRNAs (miRs) are small, noncoding RNAs that regulate the posttranscriptional expression of protein-coding mRNAs, which may have key roles in the pathogenesis of MTLE development. To study the dynamic expression patterns of brain-specific miR-124 and miR-134 and inflammation-related miR-132 and miR-21, we performed qPCR on the hippocampi of immature rats at 25 days of age. Expressions were monitored in the three stages of MTEL and in the control hippocampal tissues corresponding to the same timeframes. A similar expression method was applied to hippocampi obtained from children with MTLE and normal controls. The expression patterns of miR-124 and miR-134 nearly showed the same dynamics in the three stages of MTLE development. On the other hand, miR-132 and miR-21 showed significant upregulation in acute and chronic stages, while in the latent stage, miR-132 was upregulated and miR-21 was downregulated. The four miRs were upregulated in hippocampal tissues obtained from children with MTLE. The significant upregulation of miR-124 and miR-134 in the seizure-related stages and children suggested that both can be potential targets for anticonvulsant drugs in the epileptic developing brains, while the different expression patterns of miR-132 and miR-21 may suggest different functions in MTLE pathogenesis.
机译:颞叶颞叶癫痫(MTLE)是人类癫痫的一种特别具有毁灭性的形式,其医学难治性发生率很高。 MicroRNA(miR)是小的非编码RNA,可调节蛋白质编码mRNA的转录后表达,这可能在MTLE发病机理中起关键作用。为了研究大脑特异性miR-124和miR-134以及炎症相关miR-132和miR-21的动态表达模式,我们在25天大的未成熟大鼠海马体上进行了qPCR。在MTEL的三个阶段和对应于相同时间范围的对照海马组织中监测表达。类似的表达方法应用于从患有MTLE的儿童和正常对照中获得的海马。 miR-124和miR-134的表达模式在MTLE发育的三个阶段几乎表现出相同的动力学。另一方面,miR-132和miR-21在急性和慢性期均显示出明显的上调,​​而在潜伏期,miR-132上调而miR-21下调。从患有MTLE的儿童获得的海马组织中,四个miR上调。在癫痫发作相关阶段和儿童中,miR-124和miR-134的显着上调表明,两者都可能是癫痫发展中大脑中抗惊厥药物的潜在靶标,而miR-132和miR-21的不同表达方式可能表明在MTLE发病机理中具有不同的功能。

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