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首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >Cooperative interaction between retinoic acid receptor-alpha and estrogen receptor in breast cancer.
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Cooperative interaction between retinoic acid receptor-alpha and estrogen receptor in breast cancer.

机译:视黄酸受体α和雌激素受体在乳腺癌中的合作相互作用。

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摘要

Retinoic acid receptor-alpha (RAR alpha) is a known estrogen target gene in breast cancer cells. The consequence of RAR alpha induction by estrogen was previously unknown. We now show that RAR alpha is required for efficient estrogen receptor-alpha (ER)-mediated transcription and cell proliferation. RAR alpha can interact with ER-binding sites, but this occurs in an ER-dependent manner, providing a novel role for RAR alpha that is independent of its classic role. We show, on a genome-wide scale, that RAR alpha and ER can co-occupy regulatory regions together within the chromatin. This transcriptionally active co-occupancy and dependency occurs when exposed to the predominant breast cancer hormone, estrogen--an interaction that is promoted by the estrogen-ER induction of RAR alpha. These findings implicate RAR alpha as an essential component of the ER complex, potentially by maintaining ER-cofactor interactions, and suggest that different nuclear receptors can cooperate for effective transcriptional activity in breast cancer cells.
机译:维甲酸受体α(RAR alpha)是乳腺癌细胞中已知的雌激素靶基因。雌激素引起的RARα诱导的后果以前未知。我们现在显示RAR alpha是有效的雌激素受体alpha(ER)介导的转录和细胞增殖所必需的。 RAR alpha可以与ER结合位点相互作用,但这是以ER依赖的方式发生的,为RAR alpha提供了新颖的作用,而与它的经典作用无关。我们显示,在全基因组范围内,RAR alpha和ER可以共同占据染色质内的调节区域。当暴露于主要的乳腺癌荷尔蒙-雌激素时,就会发生这种转录活跃的共存和依赖性-这种相互作用是由雌激素-ER诱导RARα促进的。这些发现暗示RARα可能是通过维持ER-辅因子相互作用而成为ER复合物的重要组成部分,并表明不同的核受体可以协同在乳腺癌细胞中发挥有效的转录活性。

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