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首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Central amygdala nucleus (Ce) gene expression linked to increased trait-like Ce metabolism and anxious temperament in young primates
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Central amygdala nucleus (Ce) gene expression linked to increased trait-like Ce metabolism and anxious temperament in young primates

机译:中枢杏仁核(Ce)基因表达与年轻灵长类动物性状类似的Ce代谢增加和焦虑性情相关

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摘要

Children with anxious temperament (AT) are particularly sensitive to new social experiences and have increased risk for developing anxiety and depression. The young rhesus monkey is optimal for studying the origin of human AT because it shares with humans the genetic neural, and phenotypic underpinnings of complex social and emotional functioning. In vivo imaging in young monkeys demonstrated that central nucleus of the amygdala (Ce) metabolism is relatively stable across development and predicts AT. Tran-scriptome-wide gene expression, which reflects combined genetic and environmental influences, was assessed within the Ce. Results support a maladaptive neurodevelopmental hypothesis linking decreased amygdala neuroplasticity to early-life dispositional anxiety. For example, high AT individuals had decreased mRNA expression of neurotrophic tyrosine kinase, receptor, type 3 (NTRK3). Moreover, variation in Ce NTRK3 expression was inversely correlated with Ce metabolism and other AT-substrates. These data suggest that altered amygdala neuroplasticity may play a role the early dispositional risk to develop anxiety and depression.
机译:有焦虑气质(AT)的儿童对新的社交经历特别敏感,并且患焦虑和抑郁的风险增加。幼小恒河猴最适合研究人类AT的起源,因为它与人类共享复杂的社会和情感功能的遗传神经和表型基础。幼猴的体内成像显示杏仁核(Ce)代谢的中心核在整个发育过程中相对稳定并预测AT。在Ce中评估了全转录组基因表达,反映了遗传和环境的综合影响。结果支持了适应不良的神经发育假说,将杏仁核神经可塑性下降与早期生活倾向性焦虑联系起来。例如,高AT个体的神经营养性酪氨酸激酶3型受体(NTRK3)的mRNA表达下降。此外,Ce NTRK3表达的变化与Ce代谢和其他AT底物成反比。这些数据表明杏仁核神经可塑性的改变可能在早期产生焦虑和抑郁的风险中起作用。

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  • 作者

    Andrew S. Fox; Jonathan A. Oler; Steven E. Shelton; Steven A. Nanda; Richard J. Davidson; Patrick H. Roseboom; Ned H. Kalin;

  • 作者单位

    Departments of Psychology University of Wisconsin, Madison, Wl 53719 Departments of Psychiatry University of Wisconsin, Madison, Wl 53719 Waisman Laboratory for Brain Imaging and Behavior, University of Wisconsin, Madison, Wl 53705;

    Departments of HealthEmotions Research Institute, University of Wisconsin, Madison, Wl 53719Departments of Psychiatry University of Wisconsin, Madison, Wl 53719;

    Departments of HealthEmotions Research Institute, University of Wisconsin, Madison, Wl 53719Departments of Psychiatry University of Wisconsin, Madison, Wl 53719;

    Departments of Psychiatry University of Wisconsin, Madison, Wl 53719;

    Departments of Psychology University of Wisconsin, Madison, Wl 53719 Departments of HealthEmotions Research Institute, University of Wisconsin, Madison, Wl 53719 Waisman Laboratory for Brain Imaging and Behavior, University of Wisconsin, Madison, Wl 53705 Departments of Psychiatry University of Wisconsin, Madison, Wl 53719;

    Departments of Psychiatry University of Wisconsin, Madison, Wl 53719;

    Departments of Psychology University of Wisconsin, Madison, Wl 53719 Departments of HealthEmotions Research Institute, University of Wisconsin, Madison, Wl 53719 Waisman Laboratory for Brain Imaging and Behavior, University of Wisconsin, Madison, Wl 53705 Departments of Psychiatry University of Wisconsin, Madison, Wl 53719;

  • 收录信息 美国《科学引文索引》(SCI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    positron-emission tomography; microarray; brain imaging;

    机译:正电子发射断层扫描微阵列脑成像;
  • 入库时间 2022-08-18 00:40:33

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