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组织因子基因的调控

Regulation of the tissue factor gene.

作者信息

Mackman N

机构信息

Department of Immunology, Scripps Research Institute, La Jolla, California 92037, USA.

出版信息

FASEB J. 1995 Jul;9(10):883-9. doi: 10.1096/fasebj.9.10.7615158.

Abstract

The tissue factor (TF) gene is expressed in a cell type-specific manner in vivo. It is constitutively expressed by several extravascular cell types and inducibly expressed within the vasculature by monocytes and endothelial cells. TF expression initiates thrombotic episodes associated with various diseases, including atherosclerosis, septic shock, and cancer. Regulatory elements within the human TF promoter have been identified by functional analysis of TF promoter-luciferase gene plasmids transiently transfected into various cell types. Transcription factors that control expression of the TF gene were identified using gel shift mobility assays. Induction of the TF gene in human monocytic cells and endothelial cells exposed to bacterial lipopolysaccharide or cytokines is mediated by a distal enhancer (-227 to -172 bp) containing two AP-1 sites and a kappa B site. Functional interactions between Fos-Jun heterodimers and c-Rel-p65 heterodimers are required for transcriptional activation of the TF gene. In contrast, serum and phorbol ester induction of the TF gene in human epithelial cells is controlled by a proximal enhancer (-111 to +14 bp) containing three overlapping Egr-1/Sp1 binding sites. Sp1 is constitutively expressed whereas Egr-1 expression is induced by serum or phorbol ester stimulation. Sp1 also mediates basal promoter activity. Thus, TF gene expression is complex and is regulated by a number of transcription factors that bind to distinct regions of the TF promoter.

摘要

组织因子(TF)基因在体内以细胞类型特异性方式表达。它由几种血管外细胞类型组成性表达,并由单核细胞和内皮细胞在脉管系统内诱导表达。TF表达引发与多种疾病相关的血栓形成事件,包括动脉粥样硬化、脓毒性休克和癌症。通过对瞬时转染到各种细胞类型中的TF启动子-荧光素酶基因质粒进行功能分析,已鉴定出人类TF启动子内的调控元件。使用凝胶迁移率变动分析鉴定了控制TF基因表达的转录因子。暴露于细菌脂多糖或细胞因子的人类单核细胞和内皮细胞中TF基因的诱导由一个远端增强子(-227至-172 bp)介导,该增强子包含两个AP-1位点和一个κB位点。TF基因的转录激活需要Fos-Jun异二聚体和c-Rel-p65异二聚体之间的功能相互作用。相比之下,人类上皮细胞中TF基因的血清和佛波酯诱导由一个近端增强子(-111至+14 bp)控制,该增强子包含三个重叠的Egr-1/Sp1结合位点。Sp1组成性表达,而Egr-1表达由血清或佛波酯刺激诱导。Sp1还介导基础启动子活性。因此,TF基因表达很复杂,受多种与TF启动子不同区域结合的转录因子调控。

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