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T细胞中人类白细胞介素9基因的激活需要多种转录因子。

Multiple transcription factors are required for activation of human interleukin 9 gene in T cells.

作者信息

Zhu Y X, Kang L Y, Luo W, Li C C, Yang L, Yang Y C

机构信息

Walther Oncology Center, Department of Medicine, Indiana University School of Medicine, Indianapolis, Indiana 46202, USA.

出版信息

J Biol Chem. 1996 Jun 28;271(26):15815-22. doi: 10.1074/jbc.271.26.15815.

DOI:10.1074/jbc.271.26.15815
PMID:8663174
Abstract

The genetic elements and regulatory mechanisms responsible for human interleukin 9 (IL-9) gene expression in a human T cell leukemia virus type I-transformed human T cell line, C5MJ2, were investigated. We demonstrated that IL-9 gene expression is controlled, at least in part, by transcriptional activation. Transient expression of the luciferase reporter gene linked to serially deleted sequences of the 5'-flanking region of the IL-9 gene has revealed several positive and negative regulatory elements involved in the basal and inducible expression of the IL-9 gene in C5MJ2 cells. An AP-1 site at -146 to -140 was shown to be involved in the expression of the IL-9 gene. A proximal region between -46 and -80 was identified as the minimum sequence for the basal and inducible expression of the IL-9 gene in C5MJ2 cells. Within this region, an NF-kappaB site at -59 to -50 and its adjacent 20-base pair upstream sequence were demonstrated to play a critical role for the IL-9 promoter activity. DNA-protein binding studies indicated that NF-kappaB, c-Jun, and potentially novel proteins (around 35 kDa) can bind to this important sequence. Mutations at different sites within this proximal promoter region abolished the promoter activity as well as the DNA binding. Taken together, these results suggest that the cooperation of different transcription factors is essential for IL-9 gene expression in T cells.

摘要

对人I型嗜T细胞病毒转化的人T细胞系C5MJ2中负责人类白细胞介素9(IL-9)基因表达的遗传元件和调控机制进行了研究。我们证明IL-9基因表达至少部分受转录激活控制。与IL-9基因5'侧翼区串联缺失序列相连的荧光素酶报告基因的瞬时表达揭示了几个参与C5MJ2细胞中IL-9基因基础表达和诱导表达的正调控和负调控元件。-146至-140处的AP-1位点被证明与IL-9基因的表达有关。-46至-80之间的近端区域被确定为C5MJ2细胞中IL-9基因基础表达和诱导表达的最小序列。在该区域内,-59至-50处的NF-κB位点及其上游相邻的20个碱基对序列被证明对IL-9启动子活性起关键作用。DNA-蛋白质结合研究表明,NF-κB、c-Jun和潜在的新蛋白(约35 kDa)可结合到这一重要序列上。该近端启动子区域内不同位点的突变消除了启动子活性以及DNA结合。综上所述,这些结果表明不同转录因子的协同作用对于T细胞中IL-9基因表达至关重要。

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1
Multiple transcription factors are required for activation of human interleukin 9 gene in T cells.T细胞中人类白细胞介素9基因的激活需要多种转录因子。
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Human interleukin-9: genomic sequence, chromosomal location, and sequences essential for its expression in human T-cell leukemia virus (HTLV)-I-transformed human T cells.人白细胞介素-9:基因组序列、染色体定位及其在人T细胞白血病病毒(HTLV)-I转化的人T细胞中表达所必需的序列。
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