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首页> 外文期刊>The international journal of neuropsychopharmacology >Two Chronic Stress Models Based on Movement Restriction in Rats Respond Selectively to Antidepressant Drugs: Aldolase C As a Potential Biomarker
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Two Chronic Stress Models Based on Movement Restriction in Rats Respond Selectively to Antidepressant Drugs: Aldolase C As a Potential Biomarker

机译:基于运动受限的大鼠两种慢性应激模型对抗抑郁药的选择性反应:醛缩酶C作为潜在的生物标志物

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Background: Clinically depressed individuals respond to different types of antidepressants, suggesting that different neurobiological mechanisms may be responsible for their depression. However, animal models to characterize this are not yet available. Methods: We induced depressive-like behaviors in rats using 2 different chronic stress models: restraint in small cages or immobilization in adaptable plastic cones. Both models increased anxiety responses evaluated by novelty-suppressed feeding and the elevated plus-maze; increased learned helplessness evaluated by the tail suspension and forced swimming tests; and increased anhedonia evaluated by the sucrose preference test. Results: We assessed the ability of 2 different types of antidepressants to ameliorate depressive-like behaviors. We administered the serotonin reuptake inhibitor fluoxetine or the noradrenaline reuptake inhibitor reboxetine once daily for 28 days to rats that received either chronic restraint or immobilization stress, or no stress. Behavioral analysis revealed that fluoxetine ameliorated depressive-like behaviors when induced by chronic restraint stress, whereas reboxetine ameliorated these behaviors when induced by chronic immobilization stress. To further test biological differences between both models, we evaluated the levels of Aldolase C, an enzyme expressed by forebrain astrocytes that is regulated by antidepressant treatment, in the cerebrospinal fluid: chronic restraint stress, but not immobilization stress, increased the levels of Aldolase C. Moreover, the presence of astrocyte-derived Aldolase C-GFP in the cerebrospinal fluid indicates its central origin. Conclusions: Two stress paradigms induced depressive-like behaviors that were sensitive to different antidepressant treatments. Biomarkers such as Aldolase C could help determine optimal antidepressant treatments for clinically depressed patients.
机译:背景:临床上抑郁的个体对不同类型的抗抑郁药有反应,表明不同的神经生物学机制可能导致他们的抑郁。但是,尚无可用于表征此特征的动物模型。方法:我们使用两种不同的慢性应激模型在大鼠中诱发抑郁样行为:约束在小笼子中或固定在可适应的塑料锥体中。两种模型均通过新颖性抑制喂养和高迷宫评估提高了焦虑反应。通过尾部悬架和强迫游泳测试评估学习的无助感;并通过蔗糖偏爱测试评估了缺乏的快感。结果:我们评估了两种不同类型的抗抑郁药改善抑郁样行为的能力。我们对接受慢性约束或固定压力或无压力的大鼠每天一次给予血清素再摄取抑制剂氟西汀或去甲肾上腺素再摄取抑制剂瑞波西汀28天。行为分析表明,氟西汀在慢性束缚应激诱导下改善了抑郁样行为,而瑞波西汀在慢性固定应激诱导下改善了抑郁样行为。为了进一步测试两个模型之间的生物学差异,我们评估了脑脊髓液中醛缩酶C(Aldolase C)的水平,醛缩酶C是一种前脑星形胶质细胞表达的酶,该酶受抗抑郁药治疗的调节:慢性束缚压力(而非固定压力)增加了醛缩酶C的水平此外,脑脊髓液中星形胶质细胞来源的醛缩酶C-GFP的存在表明其中心来源。结论:两种应激范例诱发了对不同抗抑郁药敏感的抑郁样行为。诸如Aldolase C的生物标记物可以帮助确定临床上抑郁症患者的最佳抗抑郁药治疗方法。

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