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由转录因子GATA-1与CACCC以及AP-1/NFE-2元件相互作用产生的功能性红系启动子。

Functional erythroid promoters created by interaction of the transcription factor GATA-1 with CACCC and AP-1/NFE-2 elements.

作者信息

Walters M, Martin D I

机构信息

Fred Hutchinson Cancer Research Center, University of Washington, School of Medicine, Seattle 98104.

出版信息

Proc Natl Acad Sci U S A. 1992 Nov 1;89(21):10444-8. doi: 10.1073/pnas.89.21.10444.

Abstract

We have investigated interactions between the erythroid transcription factor GATA-1 and factors binding two cis-acting elements commonly linked to GATA sites in erythroid control elements. GATA-1 is present at all stages of erythroid differentiation, is necessary for erythropoiesis, and binds sites in all erythroid control elements. However, minimal promoters containing GATA-1 sites are inactive when tested in erythroid cells. Based on this observation, two erythroid cis elements, here termed CACCC and AP-1/NFE-2, were linked to GATA sites in minimal promoters. None of the elements linked only to a TATA box created an active promoter, but GATA sites linked to either CACCC or AP-1/NFE-2 elements formed strong erythroid promoters. A mutation of T to C at position -175 in the gamma-globin promoter GATA site, associated with hereditary persistence of fetal hemoglobin (HPFH), increased expression of these promoters in both fetal and adult cells. A construct bearing the beta-globin CACCC element was more active in adult and less active in fetal erythroid cells, when compared with the gamma-globin CACCC element. These studies suggest that erythroid control elements are formed by the interactions of at least three transcription factors, none of which functions alone.

摘要

我们研究了红系转录因子GATA-1与结合两个顺式作用元件的因子之间的相互作用,这两个顺式作用元件通常与红系控制元件中的GATA位点相连。GATA-1存在于红系分化的所有阶段,是红细胞生成所必需的,并与所有红系控制元件中的位点结合。然而,含有GATA-1位点的最小启动子在红系细胞中测试时是无活性的。基于这一观察结果,两个红系顺式元件,这里称为CACCC和AP-1/NFE-2,与最小启动子中的GATA位点相连。仅与TATA盒相连的元件均未产生活性启动子,但与CACCC或AP-1/NFE-2元件相连的GATA位点形成了强大的红系启动子。γ-珠蛋白启动子GATA位点中-175位的T到C突变与胎儿血红蛋白遗传性持续存在(HPFH)相关,增加了这些启动子在胎儿和成人细胞中的表达。与γ-珠蛋白CACCC元件相比,携带β-珠蛋白CACCC元件的构建体在成人红系细胞中更活跃,而在胎儿红系细胞中活性较低。这些研究表明,红系控制元件是由至少三种转录因子的相互作用形成的,其中没有一种转录因子单独起作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f1f4/50355/26b24c210d5a/pnas01095-0481-a.jpg

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