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多组学时代的急性应激反应。

The Acute Stress Response in the Multiomic Era.

机构信息

Laboratory of Molecular and Behavioral Neuroscience, Institute for Neuroscience, Department of Health Sciences and Technology, ETH Zürich, Switzerland; Neuroscience Center Zurich, ETH Zurich and University of Zurich, Zürich, Switzerland.

Computational Neurogenomics, Institute for Neuroscience, Department of Health Sciences and Technology, ETH Zürich, Switzerland; Neuroscience Center Zurich, ETH Zurich and University of Zurich, Zürich, Switzerland.

出版信息

Biol Psychiatry. 2021 Jun 15;89(12):1116-1126. doi: 10.1016/j.biopsych.2020.12.031. Epub 2021 Jan 13.

Abstract

Studying the stress response is a major pillar of neuroscience research not only because stress is a daily reality but also because the exquisitely fine-tuned bodily changes triggered by stress are a neuroendocrinological marvel. While the genome-wide changes induced by chronic stress have been extensively studied, we know surprisingly little about the complex molecular cascades triggered by acute stressors, the building blocks of chronic stress. The acute stress (or fight-or-flight) response mobilizes organismal energy resources to meet situational demands. However, successful stress coping also requires the efficient termination of the stress response. Maladaptive coping-particularly in response to severe or repeated stressors-can lead to allostatic (over)load, causing wear and tear on tissues, exhaustion, and disease. We propose that deep molecular profiling of the changes triggered by acute stressors could provide molecular correlates for allostatic load and predict healthy or maladaptive stress responses. We present a theoretical framework to interpret multiomic data in light of energy homeostasis and activity-dependent gene regulation, and we review the signaling cascades and molecular changes rapidly induced by acute stress in different cell types in the brain. In addition, we review and reanalyze recent data from multiomic screens conducted mainly in the rodent hippocampus and amygdala after acute psychophysical stressors. We identify challenges surrounding experimental design and data analysis, and we highlight promising new research directions to better understand the stress response on a multiomic level.

摘要

研究应激反应是神经科学研究的一个主要支柱,不仅因为应激是日常生活的现实,还因为应激引发的高度精细的身体变化是神经内分泌学的奇迹。虽然慢性应激引起的全基因组变化已经得到了广泛的研究,但我们对急性应激源引发的复杂分子级联反应,即慢性应激的构建模块,知之甚少。急性应激(或战斗或逃跑)反应调动机体的能量资源以满足情境需求。然而,成功应对压力也需要有效地终止压力反应。适应不良的应对方式——特别是对严重或反复的应激源的应对方式——会导致适应(过度)负荷,导致组织磨损、衰竭和疾病。我们提出,对急性应激源引发的变化进行深入的分子分析,可以为适应负荷提供分子相关性,并预测健康或适应不良的应激反应。我们提出了一个理论框架,根据能量平衡和活性依赖性基因调控来解释多组学数据,我们综述了不同脑区细胞类型中急性应激迅速诱导的信号级联和分子变化。此外,我们还回顾和重新分析了最近主要在啮齿动物海马体和杏仁核中进行的多组学筛选的数据分析。我们确定了围绕实验设计和数据分析的挑战,并强调了有前途的新研究方向,以更好地在多组学水平上理解应激反应。

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