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Establishment of an intermittent cold stress model using Tupaiabelangeri and evaluation of compound C737 targeting neuron-restrictive silencerfactor

机译:用Tupaia建立间歇性冷应激模型拟南芥和靶向神经元限制性沉默子的化合物C737的评价因子

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摘要

Previous studies have shown that intermittent cold stress (ICS) induces depression-like behaviors in mammals. Tupaia belangeri (the tree shrew) is the only experimental animal other than the chimpanzee that has been shown to be susceptible to infection by hepatitis B and C viruses. Moreover, full genome sequence analysis has revealed strong homology between host proteins in Tupaia and in humans and other primates. Tupaia neuromodulator receptor proteins are also known to have a high degree of homology with their corresponding primate proteins. Based on these similarities, we hypothesized that induction of ICS in Tupaia would provide a useful animal model of stress responses. We exposed young adult Tupaia to ICS and observed decreases in body temperature and body weight in both female and male Tupaia, suggesting that Tupaia are an appropriate animal model for ICS studies. We further examined the efficacy of a new small-molecule compound, C737, against the effects of ICS. C737 mimics the helical structure of neuron-restrictive silencer factor (NRSF/REST), which regulates a wide range of target genes involved in neuronal function and pain modulation. Treatment with C737 significantly reduced stress-induced weight loss in female Tupaia; these effects were stronger than those elicited by theantidepressant agomelatine. These results suggest that Tupaia representsa useful non-rodent ICS model. Our data also provide new insights into the function ofNRSF/REST in stress-induced depression and other disorders with epigenetic influences orthose with high prevalence in women.
机译:先前的研究表明,间歇性冷应激(ICS)在哺乳动物中诱发抑郁样行为。 Tupaia belangeri(树sh)是除黑猩猩以外唯一被证明容易感染乙型和丙型肝炎病毒的实验动物。此外,全基因组序列分析已经揭示了Tupaia以及人类和其他灵长类动物中宿主蛋白之间的强同源性。还已知Tupaia神经调节剂受体蛋白与其相应的灵长类蛋白具有高度同源性。基于这些相似性,我们假设在Tupaia中诱导ICS将提供一种有用的应激反应动物模型。我们将年轻的成年Tupaia暴露于ICS,观察到雌性和雄性Tupaia的体温和体重均下降,这表明Tupaia是进行ICS研究的合适动物模型。我们进一步检查了新的小分子化合物C737对抗ICS的功效。 C737模仿了神经元限制性沉默子因子(NRSF / REST)的螺旋结构,该因子调节涉及神经元功能和疼痛调节的多种靶基因。 C737治疗可显着减少雌性Tupaia引起的压力减轻体重;这些影响要强于抗抑郁药阿戈美拉汀。这些结果表明Tupaia代表有用的非啮齿动物ICS模型。我们的数据还提供了对以下功能的新见解NRSF / REST在压力诱发的抑郁症和其他具有表观遗传学影响的疾病中那些女性患病率较高的人群。

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