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早期新生期隔离会降低遭受固定应激的幼年和成年啮齿动物海马中NGF mRNA的诱导,并降低GDNF mRNA水平。

Prior neonatal isolation reduces induction of NGF mRNA and decreases GDNF mRNA in the hippocampus of juvenile and adult rodents subjected to immobilization stress.

作者信息

Kawano Ki-Ichiro, Morinobu Shigeru, Sawada Takuya, Tsuji Seiichi, Erabi Kaori, Fuchikami Manabu, Kozuru Toshiro, Yamawaki Shigeto, Hisaoka Kazue, Takebayashi Minoru

机构信息

Department of Psychiatry and Neurosciences, Hiroshima University, Minami-ku, Hiroshima, 734-8551, Japan.

出版信息

Synapse. 2008 Apr;62(4):259-67. doi: 10.1002/syn.20487.

Abstract

Numerous studies have demonstrated that early adverse experiences are associated with the development of susceptibility to stress later in life. Although it is known that early experience of adversity, such as neonatal isolation, maternal separation, and low maternal care, enhances the activity of the hypothalamo-pituitary-adrenalaxis in rodents, the detailed mechanism underlying stress susceptibility induced by early adversity remains to be elucidated. Since neurotrophins have been shown to have a neuroprotective effect, we examined the influence of repeated neonatal isolation on expression of nerve growth factor (NGF), glia cell-derived neurotrophic factor (GDNF), and neurotrophin-3 mRNA in the hippocampus of juvenile and adult rats subsequently exposed immobilization stress, using real-time quantitative PCR and in situ hybridization. Neonatal isolation did not affect the basal hippocampal expression of these neurotrophin mRNAs in either juvenile or adult rats not subsequently exposed to immobilization. Similarly, there was a significant interaction between neonatal isolation and immobilization that affected the expression of NGF and GDNF mRNAs. Neonatal isolation attenuated the induction of NGF mRNA in both groups of rats and decreased GDNF mRNA in juvenile rats in response to immobilization. The decreased induction of NGF mRNA and reduced GDNF mRNA in response to immobilization was found in the CA3 pyramidal cell layer and dentate gyrus granular cell layer in the hippocampus of adult rats that had been subjected to neonatal isolation. These findings suggest that susceptibility to stress arising from prior neonatal isolation might be a result of decreased neuroprotective support through NGF and GDNF.

摘要

大量研究表明,早期不良经历与日后生活中对应激的易感性发展有关。虽然已知早期的逆境经历,如新生鼠隔离、母婴分离和低母性关怀,会增强啮齿动物下丘脑 - 垂体 - 肾上腺轴的活性,但早期逆境诱发应激易感性的详细机制仍有待阐明。由于神经营养因子已被证明具有神经保护作用,我们使用实时定量PCR和原位杂交技术,研究了反复新生鼠隔离对随后遭受固定应激的幼年和成年大鼠海马中神经生长因子(NGF)、胶质细胞源性神经营养因子(GDNF)和神经营养因子 - 3 mRNA表达的影响。新生鼠隔离对未随后遭受固定应激的幼年或成年大鼠海马中这些神经营养因子mRNA的基础表达没有影响。同样,新生鼠隔离和固定应激之间存在显著的相互作用,影响了NGF和GDNF mRNA的表达。新生鼠隔离减弱了两组大鼠中NGF mRNA的诱导,并降低了幼年大鼠中GDNF mRNA对固定应激的反应。在经历过新生鼠隔离的成年大鼠海马的CA3锥体细胞层和齿状回颗粒细胞层中,发现对固定应激的NGF mRNA诱导减少和GDNF mRNA减少。这些发现表明,先前新生鼠隔离引起的应激易感性可能是由于通过NGF和GDNF的神经保护支持减少所致。

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