首页> 美国卫生研究院文献>International Journal of Molecular Sciences >Aberrant Early in Life Stimulation of the Stress-Response System Affects Emotional Contagion and Oxytocin Regulation in Adult Male Mice
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Aberrant Early in Life Stimulation of the Stress-Response System Affects Emotional Contagion and Oxytocin Regulation in Adult Male Mice

机译:生命早期的异常刺激应激反应系统影响成年男性小鼠的情绪传染和催产素调节

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摘要

Results over the last decades have provided evidence suggesting that HPA axis dysfunction is a major risk factor predisposing to the development of psychopathological behaviour. This susceptibility can be programmed during developmental windows of marked neuroplasticity, allowing early-life adversity to convey vulnerability to mental illness later in life. Besides genetic predisposition, also environmental factors play a pivotal role in this process, through embodiment of the mother’s emotions, or via nutrients and hormones transferred through the placenta and the maternal milk. The aim of the current translational study was to mimic a severe stress condition by exposing female CD-1 mouse dams to abnormal levels of corticosterone (80 µg/mL) in the drinking water either during the last week of pregnancy (PreCORT) or the first one of lactation (PostCORT), compared to an Animal Facility Rearing (AFR) control group. When tested as adults, male mice from PostCORT offspring and somewhat less the PreCORT mice exhibited a markedly increased corticosterone response to acute restraint stress, compared to perinatal AFR controls. Aberrant persistence of adolescence-typical increased interest towards novel social stimuli and somewhat deficient emotional contagion also characterised profiles in both perinatal-CORT groups. Intranasal oxytocin (0 or 20.0 µg/kg) generally managed to reduce the stress response and restore a regular behavioural phenotype. Alterations in density of glucocorticoid and mineralocorticoid receptors, oxytocin and µ- and κ-opioid receptors were found. Changes differed as a function of brain areas and the specific age window of perinatal aberrant stimulation of the HPA axis. Present results provided experimental evidence in a translational mouse model that precocious adversity represents a risk factor predisposing to the development of psychopathological behaviour.
机译:结果在过去几十年中提供了证据,表明HPA轴功能障碍是一种主要危险因素,涉及开发精神病理学行为。这种易感性可以在显着的神经塑性的发育窗口中编程,允许早年逆境传达生命后的精神疾病的脆弱性。除了遗传易感性之外,还通过母亲情绪的体现,或通过通过胎盘和产妇牛奶转移的营养和激素在这个过程中发挥关键作用。目前的翻译研究的目的是通过在怀孕(预先)或第一个的最后一周期间将雌性CD-1小鼠(80μg/ mL)暴露于皮质酮(80μg/ ml)的异常水平来模拟严重的应力条件。与动物设施饲养(AFR)对照组相比,哺乳期(Postcort)之一。当作为成人进行测试时,与PerinataL AFR对照相比,Postcort后代的雄性小鼠和稍微少的预制小鼠表现出显着增加的皮质酮对急性约束应激的反应。异常持续性的青春期 - 典型的新社会刺激的兴趣以及稍微缺乏情绪传染的兴趣也表征了围潜面-Colt组的特征。鼻内催产素(0或20.0μg/ kg)通常设法减少应力响应并恢复常规行为表型。发现了糖皮质激素和矿物质激素受体,催产素和μ-和κ-阿片类受体密度的改变。变化与大脑区域的函数和HPA轴的围产量刺激的特定年龄窗口不同。目前的结果提供了一种转化小鼠模型中的实验证据,以至于早期的逆境代表了危险因素,该危险因素涉及开发精神病理学行为。

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