首页> 外文期刊>The Journal of Comparative Neurology >Mossy fiber sprouting after recurrent seizures during early development in rats.
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Mossy fiber sprouting after recurrent seizures during early development in rats.

机译:大鼠早期发育期间反复发作后,苔藓纤维发芽。

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In some children, epilepsy is a catastrophic condition, leading to significant intellectual and behavioral impairment, but little is known about the consequences of recurrent seizures during development. In the present study, we evaluated the effects of 15 daily pentylenetetrazol-induced convulsions in immature rats beginning at postnatal day (P) 1, 10, or 60. In addition, we subjected another group of P10 rats to twice daily seizures for 15 days. Both supragranular and terminal sprouting in the CA3 hippocampal subfield was assessed in Timm-stained sections by using a rating scale and density measurements. Prominent sprouting was seen in the CA3 stratum pyramidale layer in all rats having 15 daily seizures, regardless of the age when seizures began. Based on Timm staining in control P10, P20, and P30 rats, the terminal sprouting in CA3 appears to be new growth of axons and synapses as opposed to a failure of normal regression of synapses. In addition to CA3 terminal sprouting, rats having twice daily seizures had sprouting noted in the dentate supragranular layer, predominately in the inferior blade of the dentate, and had a decreased seizure threshold when compared with controls. Cell counting of dentate granule cells, CA3, CA1, and hilar neurons, with unbiased stereological methods demonstrated no differences from controls in rats with daily seizures beginning at P1 or P10, whereas adult rats with daily seizures had a significant decrease in CA1 neurons. Rats that received twice daily seizures on P10-P25 had an increase in dentate granule cells. This study demonstrates that, like the mature brain, immature animals have neuronal reorganization after recurrent seizures, with mossy fiber sprouting in both the CA3 subfield and supragranular region. In the immature brain, repetitive seizures also result in granule cell neurogenesis without loss of principal neurons. Although the relationship between these morphological changes after seizures during development and subsequent cognitive impairment is not yet clear, our findings indicate that during development recurrent seizures can result in significant alterations in cell number and axonal growth.
机译:在某些儿童中,癫痫病是一种灾难性疾病,导致严重的智力和行为障碍,但对于发育过程中反复发作的后果知之甚少。在本研究中,我们评估了从出生后第1天,第10天或第60天开始,每天15次戊四氮诱发的惊厥对未成熟大鼠的惊厥的影响。此外,我们对另一组P10大鼠进行了每天两次癫痫发作,持续15天。通过使用评定量表和密度测量,在Timm染色的切片中评估了CA3海马亚区的核上和终末发芽。无论癫痫发作开始的年龄如何,在每天发作15次的所有大鼠中,CA3角锥体层均可见明显的发芽。基于对照P10,P20和P30大鼠的Timm染色,CA3的末端发芽似乎是轴突和突触的新生长,而不是突触的正常消退。除了CA3末梢发芽外,每天发作两次的大鼠在齿状上颗粒层(主要是在齿状下刀片)发芽,并且与对照组相比癫痫发作阈值降低。齿状颗粒细胞,CA3,CA1和肺门神经元的细胞计数,采用无偏见的体视学方法,发现在P1或P10开始每日发作的大鼠与对照组无差异,而每天发作的成年大鼠CA1神经元明显减少。每天两次发作P10-P25的大鼠的齿状颗粒细胞增加。这项研究表明,与成熟的大脑一样,未成熟的动物在反复发作后也会发生神经元重组,并且在CA3子域和肾上腺区域均出现苔藓纤维萌芽。在未成熟的大脑中,重复性癫痫发作还会导致颗粒细胞神经发生,而不会丢失主要神经元。尽管在发育过程中发作后这些形态学改变与随后的认知障碍之间的关系尚不清楚,但我们的发现表明,在发育过程中反复发作可导致细胞数量和轴突生长的显着改变。

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