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CRH介导的妊娠期慢性应激致子代抑郁的机制研究

CRH介导的妊娠期慢性应激致子代抑郁的机制研究
  • 导航:首页 > 科学基金
  • 批准号:81773452
  • 批准年度: 2017年
  • 学科分类:儿童少年卫生(H2606) |
  • 项目负责人:姚余有
  • 负责人职称:副教授
  • 依托单位:安徽医科大学
  • 资助金额:50万元
  • 项目类别:面上项目
  • 研究期限:2018年01月01日 至 2021年12月31日
  • 中文关键词: CRH;妊娠期;慢性;子代;抑郁
  • 英文关键词:Mental health;Growth and development and its influencing factors

项目摘要

中文摘要

抑郁症是常见疾病,是否与生命早期不良经历有关?尚未确定。已知妊娠期慢性应激致子代HPA轴紊乱,使子代促肾上腺皮质激素释放激素(CRH)升高,而过高的CRH与抑郁有关。因此,本课题拟用“中国安徽出生队列”研究妊娠期慢性应激、CRH与子代儿童抑郁的关系;利用海马、杏仁核CRHR1条件性基因敲除鼠或向子鼠侧脑室注射CRHR1拮抗剂,观察子代抑郁以及前额皮层、海马和杏仁核的病理改变,阐明CRH是否介导妊娠期慢性应激致子代抑郁;利用向子鼠侧脑室注射NMDAR拮抗剂,研究NMDAR在子代抑郁中的作用;通过观察CRHR1基因敲除、CRHR1拮抗剂和NMDAR拮抗剂对子鼠前额皮层、海马和杏仁核mTOR的影响,阐明mTOR是否参与了CRH介导的子代抑郁;通过体外培养海马脑片,加入CRH和上述受体拮抗剂并检测mTOR,进一步确认CRH是否通过NMDAR抑制mTOR的激活。该研究将为寻找防治抑郁的新途径提供资料

英文摘要

Adverse experiences during early life can potentially impact a broad range of disease in offsprings of human. For example, chronic stress during gestation can result in a reduction in birth weight and subsequently increase the likelihood of disorders of cardiovascular function, glucose homeostasis, dysregulation of hypothalamic–pituitary–adrenal (HPA) axis in offspring. Whether chronic stress during gestation could affect the onset of depression in offsprings is not determined. Previous studies showed that chronic stress during gestation could increase the level of Corticotropin-Releasing Hormone(CRH) that is considered to be related with the onset of depression in offsprings. Therefore, we will use the“China-Anhui Birth Cohort Study”to investigate the relationship among the chronic stress during gestation, the level of CRH and the depression in offsprings. In order to determine whether chronic stress during gestation-inducing the depression in offspring is mediated by CRH, hippocampal and amygdala CRH receptor1(CRHR1) gene conditional knockout mice will be used, or CRHR1-antagonist NBI30775 will be infused into the lateral ventricle. On the other hand , previous work has demonstrated that N- Methyl-D-Aspartate Receptor (NMDAR)-mediated excitotoxicity is involved in depression, and CRH-mediated spine loss required the activation of NMDAR, therefore, NMDAR-antagonist will be infused into the lateral ventricle to determine whether chronic stress during gestation-inducing the depression of offsprings is also mediated by NMDAR. . Mammalian target of rapamycin(mTOR) signals regulate neuronal survival and differentiation, dendritic arborization, axonal growth, synaptogenesis, and synaptic plasticity. Blockade of mTOR signaling completely blocked ketamine-induction of synaptogenesis and behavioral responses in models of depression. In order to determine whether mTOR is the downstream signal of CRH and NMDAR , we will compare the levels of mTOR mRNA、mTOR and p-mTOR(Ser2448)protein among CRHR1 gene conditional knockout group、CRHR1-antagonist group、NMDAR-antagonist group and control group. At last, hippocampus section will be cultured to futher determine whether CRH-mediated the downregulation of mTOR involves NMDA receptor activation. These studies will help us to explore the relationship between early life environmental exposures and the onset of depression, which will be benefit for prevention and treatment of depression.

评估说明

    国家自然科学基金项目“CRH介导的妊娠期慢性应激致子代抑郁的机制研究”发布于爱科学iikx,并永久归类于相关科学基金导航中,仅供广大科研工作者查询、学习、选题参考。国科金是根据国家发展科学技术的方针、政策和规划,以及科学技术发展方向,面向全国资助基础研究和应用研究,发挥着促进我国基础研究源头创新的作用。国科金的真正价值在于它能否为科学进步和社会发展带来积极的影响。

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