局部吗啡戒断会增加下丘脑大细胞神经分泌细胞中的c-fos基因、Fos蛋白和催产素基因的表达。
Local morphine withdrawal increases c-fos gene, Fos protein, and oxytocin gene expression in hypothalamic magnocellular neurosecretory cells.
作者信息
Johnstone L E, Brown C H, Meeren H K, Vuijst C L, Brooks P J, Leng G, Russell J A
机构信息
Department of Biomedical Sciences, University Medical School, Edinburgh, EH8 9XD, Scotland, United Kingdom.
出版信息
J Neurosci. 2000 Feb 1;20(3):1272-80. doi: 10.1523/JNEUROSCI.20-03-01272.2000.
We measured stimulation of c-fos and oxytocin gene expression during excitation of oxytocin cells induced by systemic or local morphine withdrawal. Female rats were made morphine-dependent by intracerebroventricular morphine infusion over 5 d. Morphine withdrawal, induced by systemic injection of the opioid antagonist naloxone (5 mg/kg) in conscious or anesthetized rats, increased the density of c-fos messenger RNA and of oxytocin heterogeneous nuclear RNA in supraoptic nucleus cells compared with those of nonwithdrawn rats; c-fos messenger RNA was also increased in the magnocellular and parvocellular paraventricular nuclei of withdrawn rats. Morphine withdrawal increased the number of Fos-immunoreactive cells in the supraoptic and magnocellular paraventricular nuclei of conscious or pentobarbitone-anesthetized rats. Morphine withdrawal also increased Fos-immunoreactive cell numbers in the parvocellular paraventricular nucleus of conscious but not anesthetized rats. Central administration of the alpha(1)-adrenoreceptor antagonist benoxathian (5 microg/min) did not prevent morphine withdrawal-induced increases in the numbers of Fos-immunoreactive neurons in the supraoptic or magnocellular paraventricular nucleus. Unilateral microdialysis administration of naloxone (10(-5) M) into the supraoptic nucleus of anesthetized morphine-dependent rats increased Fos-immunoreactive cell numbers compared with the contralateral nucleus. Finally, we investigated whether dependence could be induced by chronic unilateral infusion of morphine into a supraoptic nucleus; systemic naloxone (5 mg/kg) increased Fos-immunoreactive cell numbers in the morphine-infused nucleus compared with the contralateral nucleus. Thus, morphine withdrawal excitation increases c-fos and oxytocin gene expression in supraoptic nucleus neurons. This occurs independently from excitation of their ascending noradrenergic inputs, and both dependence and withdrawal can be induced within the supraoptic nucleus.
我们测量了全身或局部吗啡戒断诱导催产素细胞兴奋过程中c-fos和催产素基因表达的变化。通过脑室内注入吗啡5天使雌性大鼠产生吗啡依赖性。在清醒或麻醉大鼠中,通过全身注射阿片类拮抗剂纳洛酮(5mg/kg)诱导吗啡戒断,与未戒断大鼠相比,视上核细胞中c-fos信使核糖核酸和催产素不均一核核糖核酸的密度增加;戒断大鼠的大细胞和小细胞室旁核中c-fos信使核糖核酸也增加。吗啡戒断增加了清醒或戊巴比妥麻醉大鼠视上核和大细胞室旁核中Fos免疫反应性细胞的数量。吗啡戒断也增加了清醒但未麻醉大鼠小细胞室旁核中Fos免疫反应性细胞的数量。中枢给予α1肾上腺素能拮抗剂贝诺噻嗪(5μg/min)并不能阻止吗啡戒断诱导的视上核或大细胞室旁核中Fos免疫反应性神经元数量的增加。在麻醉的吗啡依赖性大鼠的视上核中单侧微量注射纳洛酮(10-5M),与对侧核相比,增加了Fos免疫反应性细胞的数量。最后,我们研究了慢性单侧向视上核注入吗啡是否能诱导依赖性;与对侧核相比,全身注射纳洛酮(5mg/kg)增加了注入吗啡核中Fos免疫反应性细胞的数量。因此,吗啡戒断兴奋增加了视上核神经元中c-fos和催产素基因的表达。这一过程独立于其上行去甲肾上腺素能输入的兴奋,并且依赖性和戒断都可在视上核内诱导产生。
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