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调控人类神经降压素/神经肽 N 基因表达的启动子元件的特征。

Characterization of promoter elements regulating the expression of the human neurotensin/neuromedin N gene.

机构信息

Department of Surgery, University of Texas Medical Branch, Galveston, Texas 77555, USA.

出版信息

J Biol Chem. 2011 Jan 7;286(1):542-54. doi: 10.1074/jbc.M110.145664. Epub 2010 Oct 28.

DOI:10.1074/jbc.M110.145664
PMID:21030593
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3013014/
Abstract

Expression of the gene encoding neurotensin/neuromedin N (NT/N) is mostly limited to the brain and specialized enteroendocrine N cells in the distal small intestine. We have identified key regulatory elements in the promoter region that are involved in human NT/N (hNT/N) gene expression in the novel human endocrine cell line, BON, which resembles intestinal N cells in several important aspects including NT/N precursor protein processing, ratios of different NT/N mRNA isoforms, and high levels of constitutive expression of the NT/N gene. In this study, we demonstrated multiple cis-regulatory elements including a proximal region containing a cAMP-responsive element (CRE)/AP-1-like element that binds both the AP-1 and CRE-binding protein (CREB)/ATF proteins (c-Jun, ATF-1, ATF-2, JunD, and CREB). Similar to the rat NT/N gene, this region is critical for constitutive hNT/N gene expression. Moreover, we identified a novel region that binds the orphan hormone receptor, NR2F2. We have demonstrated that the C terminus of NR2F2 strongly represses hNT/N transcription, whereas an N-terminal domain antagonizes this repressive effect. Regulation of NT/N expression by NR2F2 may have important consequences for lipid metabolism. We speculate that a complex interplay between the proximal CRE/AP-1-like motif and NR2F2 binding region exists to regulate hNT/N expression, which is critical for the high level of constitutive expression of NT/N in enteroendocrine cells. Finally, the BON cell line provides a unique model to characterize the factors regulating expression of the hNT/N gene and to better understand the mechanisms responsible for terminal differentiation of the N cell lineage in the gut.

摘要

神经降压素/神经钙素 N(NT/N)的基因表达主要局限于大脑和远端小肠的特殊肠内分泌 N 细胞。我们已经确定了启动子区域中的关键调节元件,这些元件参与了新型人内分泌细胞系 BON 中的人 NT/N(hNT/N)基因表达,该细胞系在几个重要方面类似于肠 N 细胞,包括 NT/N 前体蛋白加工、不同 NT/N mRNA 异构体的比例以及 NT/N 基因的高水平组成型表达。在这项研究中,我们证明了多个顺式调节元件,包括包含 cAMP 反应元件(CRE)/AP-1 样元件的近端区域,该元件结合了 AP-1 和 CRE 结合蛋白(CREB)/ATF 蛋白(c-Jun、ATF-1、ATF-2、JunD 和 CREB)。与大鼠 NT/N 基因相似,该区域对于组成型 hNT/N 基因表达至关重要。此外,我们确定了一个新的结合孤儿激素受体 NR2F2 的区域。我们已经证明,NR2F2 的 C 端强烈抑制 hNT/N 转录,而 N 端结构域拮抗这种抑制作用。NR2F2 对 NT/N 表达的调节可能对脂质代谢有重要影响。我们推测,近端 CRE/AP-1 样基序和 NR2F2 结合区之间存在复杂的相互作用,以调节 hNT/N 表达,这对于肠内分泌细胞中 NT/N 的高水平组成型表达至关重要。最后,BON 细胞系提供了一个独特的模型,可以用来描述调节 hNT/N 基因表达的因素,并更好地理解肠道中 N 细胞谱系终末分化的机制。

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