首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Nitric Oxide Inhibits the Transcription Repressor Yin-Yang 1 Binding Activity at the Silencer Region of the Fas Promoter:A Pivotal Role for Nitric Oxide in the Up-Regulation of Fas Gene Expression in Human Tumor Cells
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Nitric Oxide Inhibits the Transcription Repressor Yin-Yang 1 Binding Activity at the Silencer Region of the Fas Promoter:A Pivotal Role for Nitric Oxide in the Up-Regulation of Fas Gene Expression in Human Tumor Cells

机译:一氧化氮抑制Fas启动子沉默子区域的转录阻遏子Yin-Yang 1结合活性:一氧化氮在人类肿瘤细胞Fas基因表达上调中的关键作用。

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摘要

NO has been increasingly implicated in control of the transcriptional machinery and serves as an intracellular second messenger to modify gene expression. We have demonstrated that NO up-regulated Fas receptor expression in ovarian carcinoma cell lines, albeit the mechanism involved is not known. Thus, we hypothesized that NO, directly or indirectly, may modify the transcriptional machinery that is responsible for the increased expression of the Fas gene. We examined the effect of NO on Fas gene expression using a Fas promoter-driven luciferase reporter system. Transient transfection of AD10 cells with pGL-3-FasP demonstrated that the IFN-,,-dependent NO generation increases the trans-activation of the Fas promoter, and this increase was blocked by the NOS inhibitor (~.monomethyl-L-arginine), but could be restored by the addition of the NO donor S-nitroso-N-acetylpenicillamine. Systematic deletion of the Fas promoter revealed that the functional region responsible for the NO-mediated effect was located at the silencer region, suggesting that NO may be responsible for the disruption of a repressor mechanism. We demonstrate that NO up-regulates the expression of the Fas receptor on AD10 cells via the specific inactivation of the transcription repressor yin-yang 1 DNA binding activity to the silencer region of the Fas promoter. These findings reveal a new mechanism of NO-mediated gene regulation by interfering with a repressor transcription factor at the silencer region of the Fas promoter.
机译:NO已经越来越多地牵涉到转录机制的控制中,并作为细胞内第二信使来修饰基因表达。我们已经证明,尽管涉及的机制尚不清楚,但NO在卵巢癌细胞系中上调了Fas受体的表达。因此,我们假设NO可以直接或间接地修饰负责Fas基因表达增加的转录机制。我们使用Fas启动子驱动的荧光素酶报道系统检查了NO对Fas基因表达的影响。用pGL-3-FasP瞬时转染AD10细胞表明,依赖IFN的NO生成增加了Fas启动子的反式激活,而这种增加被NOS抑制剂(〜.monomethyl-L-精氨酸)阻止了。 ,但可以通过添加NO供体S-亚硝基-N-乙酰青霉胺来恢复。 Fas启动子的系统性删除表明负责NO介导的作用的功能区位于沉默区,这表明NO可能是阻遏物机制的破坏。我们证明,通过上调转录阻遏物阴阳1 DNA结合活性至Fas启动子的沉默子区域的特定失活,NO上调AD10细胞上Fas受体的表达。这些发现揭示了通过干扰Fas启动子的沉默子区域的阻遏物转录因子来NO调控基因调控的新机制。

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