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斑马鱼造血和血管发育过程中lmo2启动子的调控

Regulation of the lmo2 promoter during hematopoietic and vascular development in zebrafish.

作者信息

Zhu Hao, Traver David, Davidson Alan J, Dibiase Anthony, Thisse Christine, Thisse Bernard, Nimer Stephen, Zon Leonard I

机构信息

Division of Hematology/Oncology, Children's Hospital of Boston, Department of Pediatrics, Boston, MA 02115, USA.

出版信息

Dev Biol. 2005 May 15;281(2):256-69. doi: 10.1016/j.ydbio.2005.01.034.

Abstract

The Lmo2 transcription factor, a T-cell oncoprotein, is required for both hematopoiesis and angiogenesis. To investigate the fate of lmo2-expressing cells and the transcriptional regulation of lmo2 in vivo, we generated stable transgenic zebrafish that express green fluorescent protein (EGFP) or DsRed under the control of an lmo2 promoter. A 2.5-kb fragment contains the cis-regulatory elements required to recapitulate endogenous lmo2 expression in embryonic hematopoietic and vascular tissues. We further characterized embryonic Lmo2+ cells through transplantation into vlad tepes (vlt), an erythropoietic mutant. These Lmo2+ primitive wave donor cells differentiated into circulating hematopoietic cells and extended the life span of vlt recipients, but did not demonstrate long-term repopulation of the erythroid lineage. Promoter analysis identified a 174-bp proximal promoter that was sufficient to recapitulate lmo2 expression. This element contains critical ETS-binding sites conserved between zebrafish and pufferfish. Furthermore, we show that ets1 is coexpressed with lmo2, and overexpression experiments indicate that ets1 can activate the lmo2 promoter through this element. Our studies elucidate the transcriptional regulation of this key transcription factor, and provide a transgenic system for the functional analysis of blood and blood vessels in zebrafish.

摘要

Lmo2转录因子是一种T细胞癌蛋白,对造血和血管生成均至关重要。为了研究表达lmo2的细胞的命运以及lmo2在体内的转录调控,我们构建了稳定的转基因斑马鱼,其在lmo2启动子的控制下表达绿色荧光蛋白(EGFP)或DsRed。一个2.5 kb的片段包含在胚胎造血和血管组织中重现内源性lmo2表达所需的顺式调控元件。我们通过移植到vlad tepes(vlt)(一种红细胞生成突变体)中进一步对胚胎Lmo2 +细胞进行了表征。这些Lmo2 +原始波供体细胞分化为循环造血细胞并延长了vlt受体的寿命,但未显示出红系谱系的长期重建。启动子分析确定了一个174 bp的近端启动子,该启动子足以重现lmo2的表达。该元件包含斑马鱼和河豚之间保守的关键ETS结合位点。此外,我们表明ets1与lmo2共表达,过表达实验表明ets1可以通过该元件激活lmo2启动子。我们的研究阐明了这个关键转录因子的转录调控,并为斑马鱼血液和血管的功能分析提供了一个转基因系统。

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