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首页> 外文期刊>The Journal of biological chemistry >Characterization of the Core Mammalian Clock Component, NPAS2, as a REV-ERBα/RORα Target Gene
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Characterization of the Core Mammalian Clock Component, NPAS2, as a REV-ERBα/RORα Target Gene

机译:表征核心哺乳动物时钟组分NPAS2,作为Rev-Erbα/RORα靶基因

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摘要

The mammalian clock is regulated at the cellular level by a transcriptional/translational feedback loop. BMAL1/CLOCK (or NPAS2) heterodimers activate the expression of the PERIOD (PER) and CRYPTOCHROME (CRY) genes acting as transcription factors directed to the PER and CRY promoters via E-box elements. PER and CRY proteins form heterodimers and suppress the activity of the BMAL1/CLOCK (or NPAS2) completing the feedback loop. The circadian expression of BMAL1 is influenced by retinoic acid receptor-related orphan receptor α (RORα) and REV-ERBα, two nuclear receptors that target a ROR-response element in the promoter of the BMAL1 gene. Given that BMAL1 functions as an obligate heterodimer with either CLOCK or NPAS2, it is unclear how the expression of the partner is coordinated with BMAL1 expression. Here, we demonstrate that NPAS2 is also a RORα and REV-ERBα target gene. Using a ChIP/microarray screen, we identified both RORα and REV-ERBα occupancy of the NPAS2 promoter. We identified two functional ROREs within the NPAS2 promoter and also demonstrate that both RORα and REV-ERBα regulate the expression of NPAS2 mRNA. These data suggest a mechanism by which RORα and REV-ERBα coordinately regulate the expression of the positive arm of the circadian rhythm feedback loop.
机译:哺乳动物时钟通过转录/翻译反馈回路在蜂窝水平处调节。 BMA11 /时钟(或NPAS2)异二聚体激活时期(每个)和加密色谱(Cry)基因的表达,其作为转录因子通过电子盒元素引用靶向的转录因子。每次和乳蛋白形成异二聚体并抑制完成反馈回路的BMA1 /时钟(或NPAS2)的活性。 BMA11的昼夜节律表达受视黄酸受体相关的孤儿受体α(RORα)和REV-ERBα的影响,其靶向BMA11基因的启动子中的ROL反应元件的两个核受体。鉴于BMAL1用作钟表或NPAS2的迫使异二聚体,目前尚不清楚伴侣的表达与BMA11表达是如何协调的。这里,我们证明NPAS2也是RORα和REV-ERBα靶基因。使用芯片/微阵列筛网,我们确定了NPAS2启动子的RORα和REV-ERBα占用。我们鉴定了NPAS2启动子内的两个功能性血液,并证明RORα和REV-ERBα调节NPAS2 mRNA的表达。这些数据建议了RORα和REV-ERBα协调地调节昼夜节律反馈回路的正臂的表达的机制。

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