Effects of Chronic Stress on Prefrontal Cortex Transcriptome in Mice Displaying Different Genetic Backgrounds

被引:0
|
作者
Pawel Lisowski
Marek Wieczorek
Joanna Goscik
Grzegorz R. Juszczak
Adrian M. Stankiewicz
Lech Zwierzchowski
Artur H. Swiergiel
机构
[1] Polish Academy of Sciences,Department of Molecular Biology, Institute of Genetics and Animal Breeding
[2] University of Lodz,Department of Neurobiology, Faculty of Biology and Environmental Protection
[3] Medical University of Bialystok,Centre for Experimental Medicine
[4] Bialystok Technical University,Department of Software Engineering
[5] Polish Academy of Sciences,Department of Animal Behavior, Institute of Genetics and Animal Breeding
[6] Gdansk University,Department of Animal Physiology, Institute of Biology
来源
Journal of Molecular Neuroscience | 2013年 / 50卷
关键词
Analgesia; Chronic mild stress; Gene expression; Microarray; Mouse; Pain; Prefrontal cortex; Transcriptome; Transthyretin;
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学科分类号
摘要
There is increasing evidence that depression derives from the impact of environmental pressure on genetically susceptible individuals. We analyzed the effects of chronic mild stress (CMS) on prefrontal cortex transcriptome of two strains of mice bred for high (HA)and low (LA) swim stress-induced analgesia that differ in basal transcriptomic profiles and depression-like behaviors. We found that CMS affected 96 and 92 genes in HA and LA mice, respectively. Among genes with the same expression pattern in both strains after CMS, we observed robust upregulation of Ttr gene coding transthyretin involved in amyloidosis, seizures, stroke-like episodes, or dementia. Strain-specific HA transcriptome affected by CMS was associated with deregulation of genes involved in insulin secretion (Acvr1c, Nnat, and Pfkm), neuropeptide hormone activity (Nts and Trh), and dopamine receptor mediated signaling pathway (Clic6, Drd1a, and Ppp1r1b). LA transcriptome affected by CMS was associated with genes involved in behavioral response to stimulus (Fcer1g, Rasd2, S100a8, S100a9, Crhr1, Grm5, and Prkcc), immune effector processes (Fcer1g, Mpo, and Igh-VJ558), diacylglycerol binding (Rasgrp1, Dgke, Dgkg, and Prkcc), and long-term depression (Crhr1, Grm5, and Prkcc) and/or coding elements of dendrites (Crmp1, Cntnap4, and Prkcc) and myelin proteins (Gpm6a, Mal, and Mog). The results indicate significant contribution of genetic background to differences in stress response gene expression in the mouse prefrontal cortex.
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页码:33 / 57
页数:24
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