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严重精神障碍患者单核细胞中 TREM-1 和 DAP12 的表达。EGR3、ATF3 和 PU.1 作为重要的转录因子。

TREM-1 and DAP12 expression in monocytes of patients with severe psychiatric disorders. EGR3, ATF3 and PU.1 as important transcription factors.

机构信息

Department of Immunology, Erasmus Medical Centre Rotterdam, Rotterdam, The Netherlands.

出版信息

Brain Behav Immun. 2011 Aug;25(6):1162-9. doi: 10.1016/j.bbi.2011.03.006. Epub 2011 Mar 21.

DOI:10.1016/j.bbi.2011.03.006
PMID:21421043
Abstract

INTRODUCTION

Immune activation is a characteristic of schizophrenia (SCZ), bipolar disorder (BD) and unipolar major depressive disorder (MDD). The triggering receptor expressed on myeloid cells 1 (TREM-1), its' adaptor molecule DAP12 and their transcription factor (TF) PU.1 are important key genes in inflammation and expressed in activated monocytes and microglia.

AIM

To test: (1) if the expressions of TREM-1, DAP12 and PU.1 are increased in monocytes of patients with severe psychiatric disorders and (2) if PU.1 and the TFs ATF3 and EGR3 (which have been found as prominent increased monocyte genes in previous studies) are involved in the regulation of TREM-1 and DAP12 expression.

METHODS

Using Q-PCR, we studied the gene expression of TREM-1, DAP12, PU.1, ATF3 and EGR3 in the monocytes of 73 patients with severe psychiatric disorders (27 recent onset SCZ patients, 22 BD patients and 24 MDD patients) and of 79 healthy controls (HC). Using in silico TF binding site prediction and in vivo chromatin immunoprecipitation (ChIP), we studied the actual binding of EGR3, ATF3 and PU.1 to the promoter regions of TREM-1 and DAP12.

RESULTS

  1. TREM-1 gene expression was increased in the monocytes of SCZ and BD patients and tended to be increased in the monocytes of MDD patients. 2. DAP12 gene levels were neither increased in the monocytes of SCZ, BD, nor MDD patients. 3. PU.1 expression levels were increased in the monocytes of MDD patients, but not in those of SCZ and BD patients. 4. TREM-1 expression levels correlated in particular to ATF3 and EGR3 expression levels, DAP12 expression levels correlated in particular to PU.1 expression levels. 5. We found using binding site prediction and ChIP assays that the TFs EGR3 and ATF3 indeed bound to the TREM-1 promoter, PU.1 bound to both the TREM-1 and DAP12 promoter.

CONCLUSION

In this study, we provide evidence that TREM-1 gene expression is significantly increased in monocytes of SCZ and BD patients and that the TREM-1 gene is a target gene of the TFs ATF3 and EGR3. In MDD patients, PU.1 gene expression was increased with a tendency for TREM-1 gene over expression. Our observations support the concept that monocytes are in a pro-inflammatory state in severe psychiatric conditions and suggest differences in monocyte inflammatory set points between SCZ, BD and MDD.

摘要

简介

免疫激活是精神分裂症(SCZ)、双相情感障碍(BD)和单相重性抑郁障碍(MDD)的特征。髓样细胞表达的触发受体 1(TREM-1)、其衔接分子 DAP12 和它们的转录因子(TF)PU.1 是炎症中的重要关键基因,在激活的单核细胞和小胶质细胞中表达。

目的

检测:(1)严重精神疾病患者的单核细胞中 TREM-1、DAP12 和 PU.1 的表达是否增加,(2)TF ATF3 和 EGR3(先前研究中发现的单核细胞中显著增加的基因)是否参与 TREM-1 和 DAP12 表达的调节。

方法

使用 Q-PCR,我们研究了 73 名严重精神疾病患者(27 名近期发病的 SCZ 患者、22 名 BD 患者和 24 名 MDD 患者)和 79 名健康对照者(HC)单核细胞中 TREM-1、DAP12、PU.1、ATF3 和 EGR3 的基因表达。使用 TF 结合位点预测和体内染色质免疫沉淀(ChIP),我们研究了 EGR3、ATF3 和 PU.1 与 TREM-1 和 DAP12 启动子区域的实际结合。

结果

  1. SCZ 和 BD 患者的单核细胞中 TREM-1 基因表达增加,MDD 患者的单核细胞中 TREM-1 基因表达增加趋势。2. 单核细胞中 SCZ、BD 或 MDD 患者的 DAP12 基因水平均未增加。3. MDD 患者单核细胞中 PU.1 表达水平升高,而 SCZ 和 BD 患者单核细胞中无此现象。4. TREM-1 表达水平与 ATF3 和 EGR3 表达水平特别相关,DAP12 表达水平与 PU.1 表达水平特别相关。5. 我们通过结合位点预测和 ChIP 实验发现,TF EGR3 和 ATF3 确实与 TREM-1 启动子结合,PU.1 与 TREM-1 和 DAP12 启动子结合。

结论

在这项研究中,我们提供了证据表明,SCZ 和 BD 患者的单核细胞中 TREM-1 基因表达显著增加,TREM-1 基因是 TF ATF3 和 EGR3 的靶基因。在 MDD 患者中,PU.1 基因表达增加,TREM-1 基因表达呈过度表达趋势。我们的观察结果支持这样一种观点,即单核细胞在严重精神疾病中处于促炎状态,并表明 SCZ、BD 和 MDD 之间单核细胞炎症起始点存在差异。

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