Zhu Meng-Yang, Wang Wei-Ping, Huang Jingjing, Regunathan Soundar
Department of Pharmacology, Quillen College of Medicine, East Tennessee State University, Johnson City, Tennessee, USA.
J Neurochem. 2007 Dec;103(5):1811-20. doi: 10.1111/j.1471-4159.2007.04867.x. Epub 2007 Aug 30.
In the present study, we examined the possible effect of chronic treatment with glucocorticoids on the morphology of the rat brain and levels of endogenous agmatine and arginine decarboxylase (ADC) protein, the enzyme essential for agmatine synthesis. Seven-day treatment with dexamethasone, at a dose (10 and 50 mug/kg/day) associated to stress effects contributed by glucocorticoids, did not result in obvious morphologic changes in the medial prefrontal cortex and hippocampus, as measured by immunocytochemical staining with beta-tubulin III. However, 21-day treatment (50 mug/kg/day) produced noticeable structural changes such as the diminution and disarrangement of dendrites and neurons in these areas. Simultaneous treatment with agmatine (50 mg/kg/day) prevented these morphological changes. Further measurement with HPLC showed that endogenous agmatine levels in the prefrontal cortex and hippocampus were significantly increased after 7-day treatments with dexamethasone in a dose-dependent manner. On the contrary, 21-day treatment with glucocorticoids robustly reduced agmatine levels in these regions. The treatment-caused biphasic alterations of endogenous agmatine levels were also seen in the striatum and hypothalamus. Interestingly, treatment with glucocorticoids resulted in a similar change of ADC protein levels in most brain areas to endogenous agmatine levels: an increase after 7-day treatment versus a reduction after 21-day treatment. These results demonstrated that agmatine has neuroprotective effects against structural alterations caused by glucocorticoids in vivo. The parallel alterations in the endogenous agmatine levels and ADC expression in the brain after treatment with glucocorticoids indicate the possible regulatory effect of these stress hormones on the synthesis and metabolism of agmatine in vivo.
在本研究中,我们检测了长期使用糖皮质激素治疗对大鼠脑形态以及内源性胍丁胺和精氨酸脱羧酶(ADC,胍丁胺合成所必需的酶)蛋白水平的可能影响。地塞米松以与糖皮质激素所致应激效应相关的剂量(10和50μg/kg/天)进行7天治疗,通过β-微管蛋白III免疫细胞化学染色检测,内侧前额叶皮质和海马未出现明显形态学变化。然而,21天治疗(50μg/kg/天)产生了明显的结构变化,如这些区域的树突和神经元减少及排列紊乱。同时用胍丁胺(50mg/kg/天)治疗可预防这些形态学变化。进一步用高效液相色谱法检测显示,地塞米松7天治疗后,前额叶皮质和海马中的内源性胍丁胺水平以剂量依赖方式显著升高。相反,糖皮质激素21天治疗使这些区域的胍丁胺水平大幅降低。纹状体和下丘脑也出现了治疗引起的内源性胍丁胺水平的双相变化。有趣的是,糖皮质激素治疗导致大多数脑区的ADC蛋白水平变化与内源性胍丁胺水平相似:7天治疗后升高,21天治疗后降低。这些结果表明,胍丁胺对糖皮质激素在体内引起的结构改变具有神经保护作用。糖皮质激素治疗后大脑内源性胍丁胺水平和ADC表达的平行变化表明,这些应激激素可能在体内对胍丁胺的合成和代谢具有调节作用。