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外周胆碱酯酶抑制作用可调节处于应激状态小鼠的脑单胺水平及c-fos癌基因。

Peripheral ChE inhibition modulates brain monoamines levels and c-fos oncogene in mice subjected to a stress situation.

作者信息

Taysse L, Christin D, Delamanche S, Bellier B, Breton P

机构信息

Centre études du Bouchet (Defence Research Center), 91710, Vert le Petit, France.

出版信息

Neurochem Res. 2005 Mar;30(3):391-402. doi: 10.1007/s11064-005-2614-3.

Abstract

The present study examined, in mice, whether regional patterns of brain monoamines concentrations (DA, 5-HT and their metabolites) and expression of c-Fos protein, that may represent a prolonged functional change in neurons, could be changed after a combined exposure to stress and the peripheral cholinesterase reversible inhibitor pyridostigmine (PYR). Animals were subjected every day to a random combination of mild unescapable electric footshocks and immobilization over a 12-day period, resulting in a significant increase of glucocorticoids levels and an activation of c-fos in hippocampus, thalamus and piriform cortex. This stress protocol induced a significant increase of 5-HT levels in striatum, hippocampus and ponto mesencephalic area (PMA) but failed to induce any DA activation. When PYR (0.2 mg/kg s.c. inducing 19-35% inhibition of the plasmatic ChE activity) was administered twice a day during the last 5 days of the stress session, 5-HIAA levels and expression of c-fos oncogene were significantly increased in the most of the brain areas studied. DA levels were also enhanced in striatum/hippocampus as a result of a possible activation of mesolimbic and nigrostriatal dopamine systems. Taken together, these results suggest that a combined exposure to certain stress conditions and PYR leads, in mice, to functional changes in neurons and may affect centrally controlled functions. The mechanisms underlying these modifications and their behavioral implications remain to be further investigated.

摘要

本研究在小鼠中检测了,联合暴露于应激和外周胆碱酯酶可逆抑制剂吡啶斯的明(PYR)后,脑单胺浓度(多巴胺、5-羟色胺及其代谢产物)的区域模式以及可能代表神经元长期功能变化的c-Fos蛋白表达是否会发生改变。在12天的时间里,每天对动物进行轻度不可逃避的电足底电击和固定的随机组合,导致糖皮质激素水平显著升高以及海马体、丘脑和梨状皮质中c-fos激活。这种应激方案导致纹状体、海马体和脑桥中脑区域(PMA)的5-羟色胺水平显著升高,但未能诱导任何多巴胺激活。当在应激期的最后5天每天两次给予PYR(0.2mg/kg皮下注射,导致血浆胆碱酯酶活性抑制19-35%)时,在大多数研究的脑区中,5-羟吲哚乙酸水平和c-fos癌基因的表达显著增加。由于中脑边缘和黑质纹状体多巴胺系统可能被激活,纹状体/海马体中的多巴胺水平也有所提高。综上所述,这些结果表明,联合暴露于某些应激条件和PYR会导致小鼠神经元功能发生变化,并可能影响中枢控制的功能。这些改变的潜在机制及其行为影响仍有待进一步研究。

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