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首页> 外文期刊>Journal of molecular cell biology >Thymine DNA glycosylase promotes transactivation of β-catenin/TCFs by cooperating with CBP.
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Thymine DNA glycosylase promotes transactivation of β-catenin/TCFs by cooperating with CBP.

机译:胸腺嘧啶脱氧核糖核酸糖基化酶与CBP协同促进β-catenin/ TCF的反式激活。

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摘要

Thymine DNA glycosylase (TDG), an enzyme that initiates the repair of G/T and G/U mismatches, has been lately found crucial in embryonic development to maintain epigenetic stability and facilitate the active DNA demethylation. Here we report a novel role of TDG in Wnt signaling as a transcriptional coactivator of β-catenin/TCFs complex. Our data show that TDG binds to the transcriptional factor family LEF1/TCFs and potentiates β-catenin/TCFs transactivation, while TDG depletion suppresses Wnt3a-stimulated reporter activity or target gene transcription. Next, we show that CBP, a known coactivator, is also required for TDG function through forming a cooperative complex on target promoters. Moreover, there is an elevation of TDG levels in human colon cancer tissue, and knockdown of TDG inhibits proliferation of the colon cells. Overall, our results reveal that TDG, as a new coactivator, promotes β-catenin/TCFs transactivation and functionally cooperates with CBP in canonical Wnt signaling.
机译:最近发现,胸腺嘧啶脱氧核糖核酸糖基化酶(TDG)是一种启动G / T和G / U错配修复的酶,对于维持表观遗传稳定性和促进活性DNA去甲基化至关重要。在这里,我们报告TDG在Wnt信号中作为β-catenin/ TCFs复合体的转录共激活因子的新型作用。我们的数据显示,TDG与转录因子家族LEF1 / TCFs结合并增强β-catenin/ TCFs反式激活,而TDG耗竭则抑制Wnt3a刺激的报道分子活性或靶基因转录。接下来,我们表明,通过在靶启动子上形成协同复合物,TDG功能也需要CBP(一种已知的共激活剂)。此外,人结肠癌组织中的TDG水平升高,而TDG的敲低则抑制了结肠细胞的增殖。总体而言,我们的研究结果表明,TDG作为一种新型的共激活剂,可促进β-catenin/ TCFs的反式激活,并在经典Wnt信号传导中与CBP功能配合。

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