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Differential effects of chronic stress in young-adult and old female mice: cognitive-behavioral manifestations and neurobiological correlates

慢性应激 心理学 年轻人 海马结构 神经发生 焦虑 认知 压力源 精神病理学 心情 临床心理学 神经科学 内分泌学 内科学 海马体 医学 发展心理学 精神科
作者
Amit Lotan,Tzuri Lifschytz,Gilly Wolf,Shikma Keller,Hagar Ben-Ari,P. Tatarsky,Nir Pillar,Keren Oved,Julia Sharabany,T K Merzel,Tomoya Matsumoto,Yosuke Yamawaki,Ben Mernick,Elad Avidan,Shigeto Yamawaki,Aron Weller,Noam Shomron,Bernard Lerer
出处
期刊:Molecular Psychiatry [Springer Nature]
卷期号:23 (6): 1432-1445 被引量:31
标识
DOI:10.1038/mp.2017.237
摘要

Stress-related psychopathology is highly prevalent among elderly individuals and is associated with detrimental effects on mood, appetite and cognition. Conversely, under certain circumstances repeated mild-to-moderate stressors have been shown to enhance cognitive performance in rodents and exert stress-inoculating effects in humans. As most stress-related favorable outcomes have been reported in adolescence and young-adulthood, this apparent disparity could result from fundamental differences in how aging organisms respond to stress. Furthermore, given prominent age-related alterations in sex hormones, the effect of chronic stress in aging females remains a highly relevant yet little studied issue. In the present study, female C57BL/6 mice aged 3 (young-adult) and 20-23 (old) months were subjected to 8 weeks of chronic unpredictable stress (CUS). Behavioral outcomes were measured during the last 3 weeks of the CUS protocol, followed by brain dissection for histological and molecular end points. We found that in young-adult female mice, CUS resulted in decreased anxiety-like behavior and enhanced cognitive performance, whereas in old female mice it led to weight loss, dysregulated locomotion and memory impairment. These phenotypes were paralleled by differential changes in the expression of hypothalamic insulin and melanocortin-4 receptors and were consistent with an age-dependent reduction in the dynamic range of stress-related changes in the hippocampal transcriptome. Supported by an integrated microRNA (miRNA)-mRNA expression analysis, the present study proposes that, when confronted with ongoing stress, neuroprotective mechanisms involving the upregulation of neurogenesis, Wnt signaling and miR-375 can be harnessed more effectively during young-adulthood. Conversely, we suggest that aging alters the pattern of immune activation elicited by stress. Ultimately, interventions that modulate these processes could reduce the burden of stress-related psychopathology in late life.
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