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评估原代神经元培养作为梭曼诱导神经毒性模型的作用以及美金刚作为神经保护药物的有效性。

Assessment of primary neuronal culture as a model for soman-induced neurotoxicity and effectiveness of memantine as a neuroprotective drug.

作者信息

Deshpande S S, Smith C D, Filbert M G

机构信息

Neurotoxicology Branch, USAMRICD, Aberdeen Proving Ground, MD 21010-5425, USA.

出版信息

Arch Toxicol. 1995;69(6):384-90. doi: 10.1007/s002040050188.

DOI:10.1007/s002040050188
PMID:7495376
Abstract

An in vitro mammalian model neuronal system to evaluate the intrinsic toxicity of soman and other neurotoxicants as well as the efficacy of potential countermeasures was investigated. The link between soman toxicity, glutamate hyperactivity and neuronal death in the central nervous system was investigated in primary dissociated cell cultures from rat hippocampus and cerebral neocortex. Exposure of cortical or hippocampal neurons to glutamate for 30 min produced neuronal death in almost 80% of the cells examined at 24 h. Hippocampal neurons exposed to soman for 15-120 min at 0.1 microM concentration caused almost complete inhibition (> or = 90%) of acetylcholinesterase but failed to show any evidence of effects on cell viability, indicating a lack of direct cytotoxicity by this agent. Acetylcholine (ACh, 0.1 mM), alone or in combination with soman, did not potentiate glutamate toxicity in hippocampal neurons. Memantine, a drug used for the therapy of Parkinson's disease, spasticity and other brain disorders, significantly protected hippocampal and cortical neurons in culture against glutamate and N-methyl-D-aspartate (NMDA) excitotoxicity. In rats a single dose of memantine (18 mg/kg) administered 1 h prior to a s.c. injection of a 0.9 LD50 dose of soman reduced the severity of convulsions and increased survival. Survival, however, was accompanied by neuronal loss in the frontal cortex, piriform cortex and hippocampus.

摘要

研究了一种体外哺乳动物模型神经元系统,用于评估梭曼和其他神经毒剂的内在毒性以及潜在对抗措施的效果。在来自大鼠海马体和大脑新皮质的原代解离细胞培养物中,研究了梭曼毒性、谷氨酸活性亢进与中枢神经系统神经元死亡之间的联系。将皮质或海马体神经元暴露于谷氨酸30分钟,在24小时时,几乎80%的受试细胞发生了神经元死亡。海马体神经元在0.1微摩尔浓度下暴露于梭曼15 - 120分钟,导致乙酰胆碱酯酶几乎完全抑制(≥90%),但未显示出对细胞活力有任何影响的迹象,表明该药剂缺乏直接细胞毒性。乙酰胆碱(ACh,0.1毫摩尔)单独或与梭曼联合使用,均未增强海马体神经元中的谷氨酸毒性。美金刚是一种用于治疗帕金森病、痉挛和其他脑部疾病的药物,可显著保护培养中的海马体和皮质神经元免受谷氨酸和N - 甲基 - D - 天冬氨酸(NMDA)兴奋性毒性的影响。在大鼠中,在皮下注射0.9 LD50剂量的梭曼前1小时给予单剂量美金刚(18毫克/千克),可减轻惊厥的严重程度并提高存活率。然而,存活伴随着额叶皮质、梨状皮质和海马体中的神经元损失。

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