用乙醇处理的大鼠纹状体中的生物胺,然后将它们的大脑储存在不同的温度下。

Przemyslaw Nowak, Lukasz Labus, Joanna Stabryla, Artur Durczok, Ryszard Brus, Joanna Nowicka, Jashovam Shani
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引用次数: 4

摘要

本研究的目的是探讨乙醇预处理和脑纹状体储存温度如何影响该组织中生物胺的水平。成年Wistar雄性大鼠灌胃25%乙醇(5.0 g/kg),对照组大鼠灌胃等量生理盐水。两小时后,这些老鼠被斩首,大脑被移除,纹状体被分离。每个纹状体被分成三部分:一部分立即冷冻在干冰上,保存在-70摄氏度;第二个碎片保存在家用冰箱里(+4摄氏度);24 h后,采用HPLC/ED法测定纹状体中DA、DOPAC、HVA、3-MT、5-HT、5-HIAA的水平。斩首后立即;采用气相色谱法测定乙醇预处理和盐水预处理大鼠血清中乙醇含量。我们的研究结果表明,当纹状体储存温度从-70℃升高到+4℃,再升高到+22℃时,盐水预处理大鼠纹状体DA、DOPAC和HVA水平显著下降,而纹状体5-HT和5-HIAA水平在测试温度范围内保持不变,3-MT水平波动。经乙醇预处理的大鼠纹状体DOPAC、HVA和5-HIAA水平在三种储存温度下均升高,而DA、5-HT和3-MT水平在三种温度下均降低。纹状体样品保存在+22℃时,这些下降最为显著。我们的结论是,应该关注药物和生物胺之间可能的相互作用。
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Biogenic amines in striatum of rats that had been treated with ethanol, and their brains later stored in different temperatures.

The purpose of this study was to investigate how ethanol pretreatment and storage temperatures of brain striatum affect levels of biogenic amines in this tissue. Adult Wistar male rats were injected with 25% ethanol (5.0 g/kg i.p.) while the control rats were administered i.p. with the same volume of saline. Two hours later the rats were decapitated, their brains removed, and the striatum separated. Each striatum was divided into three parts: one part was immediately frozen on dry ice and kept at -70 degrees C; a second fragment was kept in a household refrigerator (+4 degrees C); and the third fragment was kept at +22 degrees C. Twenty-four hours later, levels of DA, DOPAC, HVA, 3-MT, 5-HT, and 5-HIAA in the striatum were assayed by HPLC/ED. Immediately after decapitation; ethanol levels were assayed in the serum of ethanol-pretreated and saline-pretreated rats using gas chromatography. Our results indicate that levels of striatal DA, DOPAC, and HVA in saline-pretreated rats decreased significantly when the storage temperature of the striatum was raised from -70 degrees C, through +4 degrees C, to +22 degrees C, while levels of striatal 5-HT and 5-HIAA remained constant within the temperature range tested and levels of 3-MT fluctuated. In ethanol-pretreated rats, striatal levels of DOPAC, HVA, and 5-HIAA were increased in all three storage temperatures, while levels of DA, 5-HT, and 3-MT were decreased in those temperatures. Those decreases were most profound in striatal samples kept at +22 degrees C. We conclude that concern about possible interactions between drugs and biogenic amines should be exercised.

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