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EKLF 通过其近端启动子和新的内含子调控区域在红系分化过程中直接激活 p21WAF1/CIP1 基因。

EKLF directly activates the p21WAF1/CIP1 gene by proximal promoter and novel intronic regulatory regions during erythroid differentiation.

机构信息

Mount Sinai School of Medicine, Department of Developmental and Regenerative Biology, Box 1020, One Gustave Levy Place, New York, NY 10029, USA.

出版信息

Mol Cell Biol. 2010 Jun;30(11):2811-22. doi: 10.1128/MCB.01016-09. Epub 2010 Apr 5.

Abstract

The switch from proliferation to differentiation during the terminal stages of erythropoiesis is a tightly controlled process that relies in part on transcription factor-mediated activation of cell cycle components. EKLF is a key transcription factor that is necessary for the initial establishment of the red cell phenotype. Here, we find that EKLF also plays a role during the subsequent differentiation process, as it induces p21(WAF1/CIP1) expression independent of p53 to regulate the changes in the cell cycle underlying erythroid maturation. EKLF activates p21 not only by directly binding to an EKLF site within a previously characterized GC-rich region in the p21 proximal promoter but also by occupancy at a novel, phylogenetically conserved region that contains consensus CACCC core motifs located downstream from the p21 TATA box. Our findings demonstrate that EKLF, likely in coordination with other transcription factors, directly contributes to the complex set of events that occur at the final erythroid cell divisions and accentuates terminal differentiation directly by activation of CDK inhibitors such as p21.

摘要

在红细胞生成的终末阶段,从增殖向分化的转变是一个受到严格控制的过程,部分依赖于转录因子介导的细胞周期成分的激活。EKLF 是一种关键的转录因子,对于初始红细胞表型的建立是必需的。在这里,我们发现 EKLF 在随后的分化过程中也发挥作用,因为它独立于 p53 诱导 p21(WAF1/CIP1)的表达,以调节红细胞成熟过程中细胞周期的变化。EKLF 通过直接结合 p21 近端启动子中先前表征的富含 GC 的区域内的 EKLF 位点,以及占据包含 TATA 盒下游保守的 CACCC 核心基序的新的系统发育保守区域,来激活 p21。我们的研究结果表明,EKLF 可能与其他转录因子协调,直接参与最终的红细胞分裂过程中发生的一系列复杂事件,并通过激活 CDK 抑制剂(如 p21)直接促进终末分化。

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