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Hippocampal proteomic changes of susceptibility and resilience to depression or anxiety in a rat model of chronic mild stress

机译:在慢性轻度应激大鼠模型中海马蛋白质组学变化对抑郁症或焦虑症的敏感性和抵抗力

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摘要

Chronic stressful occurrences are documented as a vital cause of both depression and anxiety disorders. However, the stress-induced molecular mechanisms underlying the common and distinct pathophysiology of these disorders remains largely unclear. We utilized a chronic mild stress (CMS) rat model to differentiate and subgroup depression-susceptible, anxiety-susceptible, and insusceptible rats. The hippocampus was analyzed for differential proteomes by combining mass spectrometry and the isobaric tags for relative and absolute quantitation (iTRAQ) labeling technique. Out of 2593 quantified proteins, 367 were aberrantly expressed. These hippocampal protein candidates might be associated with susceptibility to stress-induced depression or anxiety and stress resilience. They provide the potential protein systems involved in various metabolic pathways as novel investigative protein targets. Further, independent immunoblot analysis identified changes in Por, Idh2 and Esd; Glo1, G6pdx, Aldh2, and Dld; Dlat, Ogdhl, Anxal, Tpp2, and Sdha that were specifically associated to depression-susceptible, anxiety-susceptible, or insusceptible groups respectively, suggesting that identical CMS differently impacted the mitochondrial and metabolic processes in the hippocampus. Collectively, the observed alterations to protein abundance profiles of the hippocampus provided significant and novel insights into the stress regulation mechanism in a CMS rat model. This might serve as the molecular basis for further studies that would contributed to a better understanding of the similarities and differences in pathophysiologic mechanisms underlying stress-induced depression or anxiety, and stress resiliency.
机译:慢性应激事件被记录为抑郁症和焦虑症的重要原因。然而,这些疾病的共同而独特的病理生理基础的压力诱导分子机制仍然不清楚。我们利用慢性轻度应激(CMS)大鼠模型来区分抑郁症易感性,焦虑性易感性和不易感性大鼠,并将其分组。通过将质谱和等压标记相结合的相对和绝对定量(iTRAQ)标记技术,分析海马中的差异蛋白质组。在2593个定量蛋白质中,有367个被异常表达。这些海马蛋白候选物可能与应激引起的抑郁症或焦虑症和应激适应性有关。它们提供了参与各种代谢途径的潜在蛋白质系统,作为新的研究性蛋白质靶标。此外,独立的免疫印迹分析确定了Por,Idh2和Esd的变化。 Glo1,G6pdx,Aldh2和Dld; Dlat,Ogdhl,Anxal,Tpp2和Sdha分别与抑郁症易感人群,焦虑症易感人群或不敏感人群相关,这表明相同的CMS对海马线粒体和代谢过程的影响不同。总的来说,观察到的海马蛋白质丰度分布的变化为CMS大鼠模型中的压力调节机制提供了重要而新颖的见解。这可能作为进一步研究的分子基础,有助于更好地理解应激引起的抑郁或焦虑以及应激适应性的病理生理机制的异同。

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