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抗精神病药物治疗会改变编码脂质代谢相关蛋白的mRNA的表达。

Antipsychotic drug treatment alters expression of mRNAs encoding lipid metabolism-related proteins.

作者信息

Thomas E A, George R C, Danielson P E, Nelson P A, Warren A J, Lo D, Sutcliffe J G

机构信息

1Department of Molecular Biology, The Scripps Research Institute, La Jolla, CA, USA.

出版信息

Mol Psychiatry. 2003 Nov;8(12):983-93, 950. doi: 10.1038/sj.mp.4001425.

DOI:10.1038/sj.mp.4001425
PMID:14647396
Abstract

Using an automated PCR-based genomics approach, TOtal Gene expression Analysis (TOGA), we have examined gene expression profiles of mouse striatum and frontal cortex in response to clozapine and haloperidol drug treatment. Of 17 315 mRNAs observed, TOGA identified several groups of related molecules that were regulated by drug treatment. The expression of some genes encoding proteins involved in neurotransmission, signal transduction, oxidative stress, cell adhesion, apoptosis and proteolysis were altered in the brains of both clozapine- and haloperidol-treated mice as recognized by TOGA. Most notable was the differential expression of those genes whose products are associated with lipid metabolism. These include apolipoprotein D (apoD), the mouse homolog of oxysterol-binding protein-like protein 8 (OSBPL8), a diacylglycerol receptor (n-chimerin), and lysophosphatidic acid (LPA) acyltransferase. Real-time PCR analysis confirmed increases in the RNA expression of apoD (1.6-2.2-fold) and OSBPL8 (1.7-2.6-fold), and decreases in the RNA expression of n-chimerin (1.5-2.2-fold) and LPA acyltransferase (1.5-fold) in response to haloperidol and/or clozapine treatment. Additional molecules related to calcium homeostasis and signal transduction, as well as four sequences of previously unidentified mRNAs, were also confirmed by real-time PCR to be regulated by drug treatment. While antipsychotic drugs may affect several metabolic pathways, lipid metabolism/signaling pathways may be of particular importance in the mechanisms of antipsychotic drug action and in the pathophysiology of psychiatric disorders.

摘要

我们使用基于聚合酶链反应(PCR)的自动化基因组学方法——全基因表达分析(TOGA),检测了氯氮平和氟哌啶醇药物治疗后小鼠纹状体和额叶皮质的基因表达谱。在观察到的17315种信使核糖核酸(mRNA)中,TOGA鉴定出了几组受药物治疗调控的相关分子。TOGA识别出,在氯氮平和氟哌啶醇治疗的小鼠大脑中,一些参与神经传递、信号转导、氧化应激、细胞黏附、细胞凋亡和蛋白水解的蛋白质编码基因的表达发生了改变。最显著的是那些产物与脂质代谢相关的基因的差异表达。这些基因包括载脂蛋白D(apoD)、氧甾醇结合蛋白样蛋白8(OSBPL8)的小鼠同源物、二酰基甘油受体(n-嵌合蛋白)和溶血磷脂酸(LPA)酰基转移酶。实时PCR分析证实,氟哌啶醇和/或氯氮平治疗后,apoD(1.6至2.2倍)和OSBPL8(1.7至2.6倍)的RNA表达增加,n-嵌合蛋白(1.5至2.2倍)和LPA酰基转移酶(1.5倍)的RNA表达减少。实时PCR还证实,与钙稳态和信号转导相关的其他分子,以及四个先前未鉴定的mRNA序列,也受药物治疗调控。虽然抗精神病药物可能会影响多种代谢途径,但脂质代谢/信号通路可能在抗精神病药物作用机制和精神疾病病理生理学中尤为重要。

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