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通过比较主要精神障碍患者死后大脑的基因表达谱对双相情感障碍进行分子特征分析。

Molecular characterization of bipolar disorder by comparing gene expression profiles of postmortem brains of major mental disorders.

作者信息

Iwamoto K, Kakiuchi C, Bundo M, Ikeda K, Kato T

机构信息

Laboratory for Molecular Dynamics of Mental Disorders, Brain Science Institute, Saitama, Japan.

出版信息

Mol Psychiatry. 2004 Apr;9(4):406-16. doi: 10.1038/sj.mp.4001437.

Abstract

We performed the oligonucleotide microarray analysis in bipolar disorder, major depression, schizophrenia, and control subjects using postmortem prefrontal cortices provided by the Stanley Foundation Brain Collection. By comparing the gene expression profiles of similar but distinctive mental disorders, we explored the uniqueness of bipolar disorder and its similarity to other mental disorders at the molecular level. Notably, most of the altered gene expressions in each disease were not shared by one another, suggesting the molecular distinctiveness of these mental disorders. We found a tendency of downregulation of the genes encoding receptor, channels or transporters, and upregulation of the genes encoding stress response proteins or molecular chaperons in bipolar disorder. Altered expressions in bipolar disorder shared by other mental disorders mainly consisted of upregulation of the genes encoding proteins for transcription or translation. The genes identified in this study would be useful for the understanding of the pathophysiology of bipolar disorder, as well as the common pathophysiological background in major mental disorders at the molecular level. In addition, we found the altered expression of LIM and HSPF1 both in the brains and lymphoblastoid cells in bipolar disorder. These genes may have pathophysiological importance and would be novel candidate genes for bipolar disorder.

摘要

我们使用由斯坦利基金会脑库提供的死后前额叶皮质,对双相情感障碍、重度抑郁症、精神分裂症患者及对照受试者进行了寡核苷酸微阵列分析。通过比较相似但不同的精神障碍的基因表达谱,我们在分子水平上探究了双相情感障碍的独特性及其与其他精神障碍的相似性。值得注意的是,每种疾病中大多数改变的基因表达彼此并不相同,这表明这些精神障碍在分子层面具有独特性。我们发现,在双相情感障碍中,编码受体、通道或转运蛋白的基因有下调趋势,而编码应激反应蛋白或分子伴侣的基因有上调趋势。双相情感障碍中与其他精神障碍共有的表达改变主要包括编码转录或翻译相关蛋白的基因上调。本研究中鉴定出的基因将有助于理解双相情感障碍的病理生理学,以及在分子水平上理解主要精神障碍的共同病理生理背景。此外,我们发现双相情感障碍患者的大脑和淋巴母细胞中LIM和HSPF1的表达均发生了改变。这些基因可能具有病理生理学重要性,将成为双相情感障碍的新型候选基因。

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