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内皮细胞中内皮糖蛋白的表达受作用于启动子和一个-8kb增强子的Fli-1、Erg和Elf-1调控。

Endoglin expression in the endothelium is regulated by Fli-1, Erg, and Elf-1 acting on the promoter and a -8-kb enhancer.

作者信息

Pimanda John E, Chan W Y Iris, Donaldson Ian J, Bowen Mark, Green Anthony R, Göttgens Berthold

机构信息

Department of Hematology, Cambridge Institute of Medical Research, University of Cambridge, Cambridge CB2 2XY, UK.

出版信息

Blood. 2006 Jun 15;107(12):4737-45. doi: 10.1182/blood-2005-12-4929. Epub 2006 Feb 16.

Abstract

Angiogenesis is critical to the growth and regeneration of tissue but is also a key component of tumor growth and chronic inflammatory disorders. Endoglin plays a key role in angiogenesis by modulating cellular responses to transforming growth factor-beta (TGF-beta) signaling and is upregulated in proliferating endothelial cells. To gain insights into the transcriptional hierarchies that govern endoglin expression, we used a combination of comparative genomic, biochemical, and transgenic approaches. Both the promoter and a region 8 kb upstream of exon 1 were active in transfection assays in endothelial cells. In transgenic mice, the promoter directed low-level expression to a subset of endothelial cells. By contrast, inclusion of the -8 enhancer resulted in robust endothelial activity with additional staining in developing ear mesenchyme. Subsequent molecular analysis demonstrated that both the -8 enhancer and the promoter depend on conserved Ets sites, which were bound in endothelial cells in vivo by Fli-1, Erg, and Elf-1. This study therefore establishes the transcriptional framework within which endoglin functions during angiogenesis.

摘要

血管生成对于组织的生长和再生至关重要,但也是肿瘤生长和慢性炎症性疾病的关键组成部分。内皮糖蛋白通过调节细胞对转化生长因子-β(TGF-β)信号的反应在血管生成中起关键作用,并且在增殖的内皮细胞中上调。为了深入了解控制内皮糖蛋白表达的转录层次结构,我们结合了比较基因组学、生物化学和转基因方法。启动子和外显子1上游8 kb的区域在内皮细胞的转染试验中均具有活性。在转基因小鼠中,启动子将低水平表达导向一部分内皮细胞。相比之下,包含-8增强子导致强大的内皮活性,并在发育中的耳部间充质中出现额外染色。随后的分子分析表明,-8增强子和启动子均依赖于保守的Ets位点,这些位点在体内的内皮细胞中被Fli-1、Erg和Elf-1结合。因此,本研究建立了内皮糖蛋白在血管生成过程中发挥作用的转录框架。

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