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首页> 外文期刊>Scientific reports. >Metastasis-associated protein 1 is an upstream regulator of DNMT3a and stimulator of insulin-growth factor binding protein-3 in breast cancer
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Metastasis-associated protein 1 is an upstream regulator of DNMT3a and stimulator of insulin-growth factor binding protein-3 in breast cancer

机译:转移相关蛋白1是乳腺癌中胰岛素 - 生长因子结合蛋白-3的DNMT3A和刺激器的上游调节剂

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摘要

Despite a recognized role of DNA methyltransferase 3a (DNMT3a) in human cancer, the nature of its upstream regulator(s) and relationship with the master chromatin remodeling factor MTA1, continues to be poorly understood. Here, we found an inverse relationship between the levels of MTA1 and DNMT3a in human cancer and that high levels of MTA1 in combination of low DNMT3a status correlates well with poor survival of breast cancer patients. We discovered that MTA1 represses DNMT3a expression via HDAC1/YY1 transcription factor complex. Because IGFBP3 is an established target of DNMT3a, we investigated the effect of MTA1 upon IGFBP3 expression, and found a coactivator role of MTA1/c-Jun/Pol II coactivator complex upon the IGFBP3 transcription. In addition, MTA1 overexpression correlates well with low levels of DNMT3a which, in turn also correlates with a high IGFBP3 status in breast cancer patients and predicts a poor clinical outcome for breast cancer patients. These findings suggest that MTA1 could regulate the expression of IGFBP3 in both DNMT3a-dependent and -independent manner. Together findings presented here recognize an inherent role of MTA1 as a modifier of DNMT3a and IGFBP3 expression, and consequently, the role of MTA1-DNMT3a-IGFBP3 axis in breast cancer progression.
机译:尽管DNA甲基转移酶3a(DNMT3A)在人类癌症中具有公认的作用,但其上游调节剂的性质和与总染色质重塑因子MTA1的关系仍然明白差不多。在这里,我们发现人类癌症中MTA1和DNMT3a水平与低水平的MTA1之间的反比关系,低DNMT3A状态的组合与乳腺癌患者的不良存活率良好。我们发现MTA1通过HDAC1 / YY1转录因子复合体压抑DNMT3A表达。因为IGFBP3是DNMT3A的已建立的靶标,所以我们研究了MTA1对IGFBP3表达的影响,发现MTA1 / C-JUN / POL II共酰胺络合物在IGFBP3转录上的同觉体作用。此外,MTA1过表达与低水平的DNMT3a相关,这也与乳腺癌患者的高IGFBP3状态相关,并预测乳腺癌患者的临床结果不良。这些发现表明MTA1可以以DNMT3A依赖性和依赖性方式调节IGFBP3的表达。这里介绍的结果识别MTA1作为DNMT3A和IGFBP3表达的改性剂的固有作用,因此,MTA1-DNMT3A-IGFBP3轴在乳腺癌进展中的作用。

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