首页> 美国卫生研究院文献>The Journal of Neuroscience >The Effects of Acute Nicotine on the Metabolism of Dopamine and the Expression of Fos Protein in Striatal and Limbic Brain Areas of Rats during Chronic Nicotine Infusion and Its Withdrawal
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The Effects of Acute Nicotine on the Metabolism of Dopamine and the Expression of Fos Protein in Striatal and Limbic Brain Areas of Rats during Chronic Nicotine Infusion and Its Withdrawal

机译:慢性尼古丁对慢性尼古丁输注和戒断大鼠多巴胺代谢和纹状体和边缘脑区Fos蛋白表达的影响

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摘要

The effects of acute nicotine (0.5 mg/kg, s.c.) on dopamine (DA) metabolism and Fos protein expression in striatal and limbic areas of rats on the seventh day of chronic nicotine infusion (4 mg · kg−1 · d−1) and after 24 or 72 hr withdrawal were investigated. In saline-infused rats, acute nicotine elevated striatal and limbic 3,4-dihydroxyphenylacetic acid (DOPAC) and homovanillic acid (HVA) concentrations significantly. During the nicotine infusion, no such increases were seen in the striatum, but limbic HVA was somewhat elevated. After 24 hr withdrawal when no nicotine was found in the plasma, acute nicotine elevated striatal DOPAC and HVA and limbic HVA. However, the limbic DOPAC was unaffected. Acute nicotine increased Fos immunostaining (IS) in the caudate-putamen (CPU), the core of nucleus accumbens (NAcc), the cingulate cortex (Cg), and the central nucleus of amygdala (ACe) significantly. During nicotine infusion the nicotine-induced responses were attenuated in CPU and NAcc, whereas in ACe and Cg Fos immunostaining was increased as in saline-infused rats. After 24 hr withdrawal, acute nicotine did not increase Fos immunostaining in CPU, NAcc, and Cg, but increased it clearly in ACe. After 72 hr withdrawal, nicotine’s effects were restored. Our findings suggest that the nicotinic receptors in the striatal areas are desensitized more easily than those in the limbic areas. Furthermore, the effects of nicotine on various DA metabolites differ. We also found evidence for long-lasting inactivation of nicotinic receptors in vivo regulating limbic dopamine metabolism and Fos expression in striatal and limbic areas. These findings might be important for the protective effects of nicotine in Parkinson’s disease and in its dependence-producing properties.
机译:慢性尼古丁输注(4 mg·kg -1)第七天,急性尼古丁(0.5 mg / kg,sc)对大鼠纹状体和边缘区多巴胺(DA)代谢和Fos蛋白表达的影响sup>·d -1 )以及停药24或72小时后进行了调查。在注入盐水的大鼠中,急性尼古丁会显着提高纹状体和边缘3,4-二羟基苯乙酸(DOPAC)和高香草酸(HVA)的浓度。在尼古丁输注过程中,纹状体中未见此类增加,但边缘HVA有所升高。停药24小时后,血浆中未发现尼古丁,急性尼古丁会升高纹状体DOPAC和HVA和边缘性HVA。但是,边缘性DOPAC不受影响。急性尼古丁显着提高尾状-丘脑(CPU),伏伏核(NAcc)的核心,扣带回皮层(Cg)和杏仁核(ACe)的中央核的Fos免疫染色(IS)。在尼古丁输注过程中,尼古丁诱导的反应在CPU和NAcc中减弱,而在ACe和Cg Fos中,免疫灌注的增加与注入盐水的大鼠相同。停药24小时后,急性尼古丁在CPU,NAcc和Cg中并未增加Fos免疫染色,而在ACe中则明显增加。停药72小时后,尼古丁的作用得以恢复。我们的发现表明,纹状体区的烟碱受体比边缘区的烟碱受体更容易脱敏。此外,尼古丁对各种DA代谢产物的作用也不同。我们还发现在体内调节纹状体和边缘区的边缘多巴胺代谢和Fos表达的烟碱受体长期失活的证据。这些发现可能对尼古丁对帕金森氏病的保护作用及其产生依赖性具有重要意义。

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