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首页> 外文期刊>Frontiers in Pharmacology >Early-Life Stress Induces Depression-Like Behavior and Synaptic-Plasticity Changes in a Maternal Separation Rat Model: Gender Difference and Metabolomics Study
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Early-Life Stress Induces Depression-Like Behavior and Synaptic-Plasticity Changes in a Maternal Separation Rat Model: Gender Difference and Metabolomics Study

机译:早期应激诱导抑郁症的行为和突触塑性变化在母体分离大鼠模型中:性别差异和代谢组学研究

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More than 300 million people suffer from depressive disorders globally. People under early-life stress (ELS) are reportedly vulnerable to depression in their adulthood, and synaptic plasticity can be the molecular mechanism underlying such depression. Herein, we simulated ELS by using a maternal separation (MS) model and evaluated the behavior of Sprague–Dawley (SD) rats in adulthood through behavioral examination, including sucrose preference, forced swimming, and open-field tests. The behavior tests showed that SD rats in the MS group were more susceptible to depression- and anxiety-like behaviors than did the non-MS (NMS) group. Nissl staining analysis indicated a significant reduction in the number of neurons at the prefrontal cortex and hippocampus, including the CA1, CA2, CA3, and DG regions of SD rats in the MS group. Immunohistochemistry results showed that the percentages of synaptophysin-positive area in the prefrontal cortex and hippocampus (including the CA1, CA2, CA3, and DG regions) slice of the MS group significantly decreased compared with those of the NMS group. Western blot analysis was used to assess synaptic-plasticity protein markers, including postsynaptic density 95, synaptophysin, and growth-associated binding protein 43 protein expression in the cortex and hippocampus. Results showed that the expression levels of these three proteins in the MS group were significantly lower than those in the NMS group. LC–MS/MS analysis revealed no significant differences in the peak areas of sex hormones and their metabolites, including estradiol, testosterone, androstenedione, estrone, estriol, and 5β-dihydrotestosterone. Through the application of nontargeted metabolomics to the overall analysis of differential metabolites, pathway-enrichment results showed the importance of arginine and proline metabolism; pantothenate and CoA biosyntheses; glutathione metabolism; and the phenylalanine, tyrosine, and tryptophan biosynthesis pathways. In summary, the MS model caused adult SD rats to be susceptible to depression, which may regulate synaptic plasticity through arginine and proline metabolism; pantothenate and CoA biosyntheses; glutathione metabolism; and phenylalanine, tyrosine, and tryptophan biosyntheses.
机译:超过3亿人患有全球抑郁症的抑郁症。据报道,人们在早期的压力(ELS)易受其成年期抑郁症,并且突触可塑性可以是这种抑郁症的分子机制。在此,我们通过使用母体分离(MS)模型来模拟ELS,并通过行为检查评估成年性的Sprague-Dawley(SD)大鼠的行为,包括蔗糖偏好,强制游泳和开放场测试。行为测试表明,MS组中的SD大鼠比非MS(NMS)组更容易受到抑郁和焦虑的行为。 NISSL染色分析表明前额叶皮质和海马的神经元数显着降低,包括MS组中的SD大鼠的CA1,CA,CA3和DG区域。免疫组织化学结果表明,与NMS组相比,MS组的前额叶皮层和海马(Ca1,Ca2,Ca3和Dg区)中突触素阳性面积的百分比显着降低。用于评估突触塑性蛋白标记物,包括突触塑性蛋白质标记物,包括突触后的密度95,突触细胞和生长相关的结合蛋白43蛋白表达在皮质和海马中。结果表明,MS组中这三种蛋白质的表达水平明显低于NMS组中的表达水平。 LC-MS / MS分析显示性激素和代谢物的峰面积没有显着差异,包括雌二醇,睾酮,雄甾酮,雌激素,雌醇和5β-二氢酮。通过将非靶向代谢组织的应用应用于差异代谢物的总体分析,致富集结果表明精氨酸和脯氨酸代谢的重要性;泛酸和CoA Biosyntheses;谷胱甘肽新陈代谢;和苯丙氨酸,酪氨酸和色氨酸生物合成途径。总之,MS模型使成年SD大鼠易受抑郁症,这可能通过精氨酸和脯氨酸代谢来调节突触塑性;泛酸和CoA Biosyntheses;谷胱甘肽新陈代谢;和苯丙氨酸,酪氨酸和色氨酸生物合成。

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