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转录抑制因子Nkx6.1在胰腺β细胞分化过程中也作为一种依赖于脱氧核糖核酸环境的转录激活因子发挥作用:Nkx6.1对nkx6.1基因进行反馈激活的证据。

The transcriptional repressor Nkx6.1 also functions as a deoxyribonucleic acid context-dependent transcriptional activator during pancreatic beta-cell differentiation: evidence for feedback activation of the nkx6.1 gene by Nkx6.1.

作者信息

Iype Tessy, Taylor David G, Ziesmann Suzanne M, Garmey James C, Watada Hirotaka, Mirmira Raghavendra G

机构信息

Department of Internal Medicine, University of Virginia Health System, Charlottesville, Virginia 22903, USA.

出版信息

Mol Endocrinol. 2004 Jun;18(6):1363-75. doi: 10.1210/me.2004-0006. Epub 2004 Mar 31.

Abstract

In the pancreas, the NK homeodomain transcription factor Nkx6.1 is required for the development of beta-cells and is believed to function as a potent repressor of transcription upon binding to A/T-rich sequences within the promoter region of target genes. Because the nkx6.1 promoter itself contains several such sequences, we considered the possibility that the expression level and restricted pattern of the nkx6.1 gene might be precisely regulated by one or more homeodomain transcription factors, including Nkx6.1 itself. In this report, we identify a novel beta-cell-specific enhancer element in the nkx6.1 gene between -157 and -30 bp (relative to the transcriptional start site) that harbors a conserved A/T-containing sequence flanked by G/C-rich stretches. Although the islet homeodomain-containing activator Pdx-1 was unable to stimulate transcription of a reporter gene through this enhancer element in mammalian cell lines, strikingly, Nkx6.1 robustly activated transcription through direct interaction with the A/T-rich sequence in this element. We demonstrate that this activation is indeed transcriptional in nature (and not secondary to translational effects) and is mediated by a modular acidic sequence within the COOH-terminal domain of Nkx6.1. We show by EMSAs that Nkx6.1 binds to the beta-cell-specific enhancer in vitro and by chromatin immunoprecipitation assays that Nkx6.1 natively occupies this region in vivo in betaTC3 cells. We therefore conclude that Nkx6.1 is a bifunctional transcription factor that serves to maintain the specific expression of its own gene during beta-cell differentiation while simultaneously effecting broader gene repression events.

摘要

在胰腺中,NK 同源异型结构域转录因子 Nkx6.1 是β细胞发育所必需的,并且据信在与靶基因启动子区域内富含 A/T 的序列结合后,它作为一种强大的转录抑制因子发挥作用。由于 nkx6.1 启动子本身包含几个这样的序列,我们考虑了 nkx6.1 基因的表达水平和受限模式可能受到一个或多个同源异型结构域转录因子(包括 Nkx6.1 自身)精确调控的可能性。在本报告中,我们在 nkx6.1 基因中位于 -157 至 -30 bp(相对于转录起始位点)之间鉴定出一个新的β细胞特异性增强子元件,该元件含有一个保守的富含 A/T 的序列,两侧为富含 G/C 的片段。尽管含胰岛同源异型结构域的激活因子 Pdx-1 在哺乳动物细胞系中无法通过该增强子元件刺激报告基因的转录,但令人惊讶的是,Nkx6.1 通过与该元件中富含 A/T 的序列直接相互作用而有力地激活转录。我们证明这种激活实际上是转录性质的(而非继发于翻译效应),并且由 Nkx6.1 的 COOH 末端结构域内的一个模块化酸性序列介导。我们通过电泳迁移率变动分析表明 Nkx6.1 在体外与β细胞特异性增强子结合,并且通过染色质免疫沉淀分析表明 Nkx6.1 在体内于βTC3 细胞中天然占据该区域。因此,我们得出结论,Nkx6.1 是一种双功能转录因子,在β细胞分化过程中用于维持其自身基因的特异性表达,同时影响更广泛的基因抑制事件。

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