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首页> 外文期刊>Molecular and Cellular Biology >Estrogen-induced apoptosis by inhibition of the erythroid transcription factor GATA-1.
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Estrogen-induced apoptosis by inhibition of the erythroid transcription factor GATA-1.

机译:雌激素通过抑制类红细胞转录因子GATA-1诱导细胞凋亡。

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摘要

Steroid hormones regulate diverse biological functions, including programmed cell death (apoptosis). Although steroid receptors have been studied extensively, relatively little is known regarding the cellular targets through which apoptosis is triggered. We show here that the ligand-activated estrogen receptor (ER) induces apoptosis in an erythroid cell line by binding to, and consequently inhibiting the activity of, GATA-1, an erythroid transcription factor essential for the survival and maturation of erythroid precursor cells. GATA-1 inhibition is reflected in the downregulation of presumptive GATA-1 target genes. Constitutive overexpression of a GATA-binding protein resistant to the effects of the ER partially rescues ER-induced apoptosis. Induction of apoptosis by a mutant ER defective in binding to the estrogen response element but active in GATA-1 inhibition suggests that ER-mediated inhibition of GATA-1 is direct and does not require estrogen response element-dependent transcriptional activation. Thus, a lineage-restricted transcription factor, such as GATA-1, constitutes one cellular target through which steroid hormones may control apoptosis. As GATA-binding proteins are evolutionarily conserved, we speculate that members of the steroid receptor family may exert some of their diverse biological functions in different cellular contexts through interference with the function of GATA-binding proteins.
机译:类固醇激素调节多种生物学功能,包括程序性细胞死亡(细胞凋亡)。尽管类固醇受体已被广泛研究,但关于触发细胞凋亡的细胞靶标知之甚少。我们在这里显示,配体激活的雌激素受体(ER)通过与GATA-1结合并因此抑制其活性,该因子是红系前体细胞存活和成熟所必需的红系转录因子GATA-1,从而诱导红系细胞系中的凋亡。 GATA-1抑制作用反映在假定的GATA-1靶基因的下调中。抗ER作用的GATA结合蛋白的组成型过表达部分挽救了ER诱导的细胞凋亡。由突变的ER诱导的细胞凋亡在结合雌激素反应元件方面是缺陷的,但是在GATA-1抑制中有效,这表明ER介导的对GATA-1的抑制是直接的,不需要雌激素反应元件依赖性的转录激活。因此,谱系限制的转录因子,如GATA-1,构成了一个细胞靶标,类固醇激素可通过该靶标控制细胞凋亡。由于GATA结合蛋白在进化上是保守的,我们推测类固醇受体家族的成员可能通过干扰GATA结合蛋白的功能而在不同的细胞环境中发挥其多种生物学功能。

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