致癌同源蛋白TLX1/HOX11对人ALDH1A1启动子的转录调控

K. Rice, M. Heidari, Ross H. Taplin, U. Kees, W. Greene
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引用次数: 2

摘要

同源蛋白TLX1在未成熟T细胞中异常表达时对脾脏器官发生和肿瘤发生至关重要,它是一种双功能转录调节因子,能够根据细胞类型和/或启动子背景激活或抑制。然而,其调控靶基因(如ALDH1A1)转录的详细机制仍有待阐明。因此,我们通过荧光素酶报告细胞和迁移转移试验,从功能上评估了TLX1在两种造血细胞系(PER-117 t -白血病细胞和人红白血病(HEL)细胞)中调节ALDH1A1表达的能力。我们发现TLX1通过其同源结构域与一般转录因子TFIIB物理相互作用,并确定了TLX1介导的对含有ALDH1A1启动子的CCAAT盒的调节的两个活性。第一种方法涉及通过干扰组装在非规范TATA (GATA)盒中的含GATA因子的蛋白质复合物来抑制ccaat依赖性转录。虽然不需要直接的DNA结合,但结构完整的同源结构域是TLX1抑制所必需的。第二种活性涉及不依赖ccaat的转录激活,不需要完整的同源结构域,这表明TLX1的激活和抑制功能是不同的。这些发现证实了TLX1对ALDH1A1基因的调控,并支持TLX1功能的间接模型,其中蛋白质-蛋白质相互作用,而不是特定位点的DNA结合,对其转录活性至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Transcriptional regulation of the human ALDH1A1 promoter by the oncogenic homeoprotein TLX1/HOX11
The homeoprotein TLX1, which is essential to spleen organogenesis and oncogenic when aberrantly expressed in immature T cells, functions as a bifunctional transcriptional regulator, being capable of activation or repression depending on cell type and/or promoter context. However, the detailed mechanisms by which it regulates the transcription of target genes such as ALDH1A1 remains to be elucidated. We therefore functionally assessed the ability of TLX1 to regulate ALDH1A1 expression in two hematopoietic cell lines, PER-117 T-leukemic cells and human erythroleukemic (HEL) cells, by use of luciferase reporter and mobility shift assays. We showed that TLX1 physically interacts with the general transcription factor TFIIB via its homeodomain, and identified two activities in respect to TLX1-mediated regulation of the CCAAT box-containing ALDH1A1 promoter. The first involved CCAAT-dependent transcriptional repression via perturbation of GATA factor-containing protein complexes assembled at a non-canonical TATA (GATA) box. A structurally intact homeodomain was essential for repression by TLX1 although direct DNA binding was not required. The second activity, which involved CCAAT-independent transcriptional activation did not require an intact homeodomain, indicating that the activation and repression functions of TLX1 are distinct. These findings confirm ALDH1A1 gene regulation by TLX1 and support an indirect model for TLX1 function, in which protein-protein interactions, rather than DNA binding at specific sites, are crucial for its transcriptional activity.
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