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大剂量破伤风毒素全身给药后小鼠海马胶质增生而无神经元死亡。

Gliosis in the mouse hippocampus without neuronal death after systemic administration of high dosage of tetanus toxin.

机构信息

Department of Emergency Medicine, College of Medicine, Hallym University Sacred Heart Hospital, Hallym University, Anyang, South Korea.

出版信息

Cell Mol Neurobiol. 2012 Apr;32(3):423-34. doi: 10.1007/s10571-011-9772-4. Epub 2011 Dec 3.

Abstract

Tetanus toxin (TeT), an exotoxin, has been studied to cause tetanus in mammalian brains, and it can block the release of some neurotransmitters and affect seizure propagation. In the present study, we investigated neuronal damage/death and glial changes in the mouse hippocampus after systemic administration (intraperitoneal injection) of TeT 10 and 100 ng/kg. In both the 10 and 100 ng/kg TeT-treated groups, no neuronal death occurred in any subregions of the mouse hippocampus until 24 h post-treatment; however, there were changes in glia in the hippocampus depending on time course and dosage. The morphology of GFAP-immunoreactive astrocytes and Iba-1-immunoreactive microglia was apparently changed in the 100 ng/kg TeT treated-group compared to the 10 ng/kg TeT treated-group. In the 100 ng/kg TeT treated-group, they were increased in size and their immunoreactivity was distinctively increased from 12 h post-treatment. We also found that their protein levels were increased in the hippocampus at 12 h post-treatment of 100 ng/kg TeT. In conclusion, these results indicate that the systemic administration of 100 ng/kg TeT induced a distinctive microglia changes in the mouse hippocampus without any neuronal death/damage.

摘要

破伤风毒素(TeT)是一种外毒素,已被研究用于在哺乳动物大脑中引起破伤风,它可以阻断一些神经递质的释放并影响癫痫发作的传播。在本研究中,我们研究了 TeT 10 和 100ng/kg 全身给药(腹腔注射)后小鼠海马区的神经元损伤/死亡和神经胶质变化。在 TeT 10 和 100ng/kg 处理组中,在处理后 24 小时内,任何亚区的神经元都没有死亡;然而,根据时间过程和剂量,海马中的神经胶质发生了变化。与 10ng/kg TeT 处理组相比,100ng/kg TeT 处理组中海马中的 GFAP-免疫反应性星形胶质细胞和 Iba-1-免疫反应性小胶质细胞的形态明显改变。在 100ng/kg TeT 处理组中,从 12 小时后开始,其大小增加,免疫反应明显增强。我们还发现,在 100ng/kg TeT 处理后 12 小时,其蛋白水平在海马体中增加。总之,这些结果表明,100ng/kg TeT 的全身给药在没有任何神经元死亡/损伤的情况下,在小鼠海马区引起了独特的小胶质细胞变化。

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