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首页> 外文期刊>Oncogene >Differential regulation of PTEN expression by androgen receptor in prostate and breast cancers
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Differential regulation of PTEN expression by androgen receptor in prostate and breast cancers

机译:前列腺癌和乳腺癌中雄激素受体对PTEN表达的差异调节

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摘要

Prostate cancer and breast cancer are the most common malignancies in the western world. Androgen receptor (AR) and PTEN both have been well documented to have important roles in prostate carcinogenesis. In contrast, AR and PTEN in breast carcinogenesis have not been well studied. Furthermore, the crosstalk and connection between those two pathways remain unclear. Increased AR expression in prostate cancers, combined with decreased PTEN expression, portends a poor clinical outcome. Paradoxically, both high AR and high PTEN levels, detected by immunohistochemistry, in primary breast carcinomas have been associated with better disease-free survival. Here, we performed in silico analysis of publicly available microarray data sets from prostate or breast carcinomas. We found an inverse correlation between AR and PTEN transcript expression in prostate cancer tissues in contrast to the positive correlation in breast cancer. These data led us to hypothesize that AR may directly affect PTEN transcriptional regulation in prostate and breast cancer cells. Here, we show for the first time that AR inhibits PTEN transcription in prostate cancer cells, whereas AR upregulates PTEN transcription in breast cancer cells, which mechanistically explains both the immunohistochemical PTEN鈥揂R expressional data noted in clinical trials and in our in silico analysis of the transcriptomes of breast and prostate cancers. In addition, we have fine-mapped the AR-binding motif within the PTEN promoter. Here we show that, in patients with Cowden syndrome, an inherited cancer syndrome caused by germline mutations scattered throughout PTEN , point variants affecting the 3鈥?end of the AR-binding motif result in abrogation of androgen-mediated transcriptional regulation of PTEN expression. We may speculate that the differential AR effect on PTEN may begin to explain organ-specific and perhaps sex-specific neoplasia predisposition in Cowden syndrome, as well as why only a fraction of women with germline PTEN mutations develop breast cancer, depending on the androgen steroid milieu and levels.
机译:前列腺癌和乳腺癌是西方世界最常见的恶性肿瘤。雄激素受体(AR)和PTEN均已被证明在前列腺癌的发生中具有重要作用。相比之下,AR和PTEN在乳腺癌的致癌作用方面尚未得到很好的研究。此外,这两个路径之间的串扰和连接仍然不清楚。前列腺癌中AR表达的增加,与PTEN表达的减少相结合,预示了不良的临床结果。矛盾的是,在原发性乳腺癌中通过免疫组织化学检测到的高AR和高PTEN水平都与更好的无病生存率相关。在这里,我们对来自前列腺癌或乳腺癌的公开可用微阵列数据集进行了计算机分析。我们发现前列腺癌组织中 AR和 PTEN转录物表达之间呈负相关,而乳腺癌中呈正相关。这些数据使我们假设AR可能直接影响前列腺和乳腺癌细胞中的PTEN转录调控。在这里,我们首次展示了AR抑制前列腺癌细胞中的 PTEN转录,而AR上调了乳腺癌细胞中的 PTEN转录,这从机理上解释了临床试验中提到的免疫组化PTEN'揂R表达数据以及在我们对乳腺癌和前列腺癌的转录组进行的计算机分析中。另外,我们已经在

启动子内精细映射了AR结合基序。在这里,我们表明,在患有Cowden综合征的患者中,由散布在整个PTEN中的种系突变引起的遗传性癌症综合征,影响AR结合基序3'末端的点变异导致雄激素介导的转录调控的废止。 PTEN表达。我们可能推测,不同的AR对PTEN的作用可能开始解释了Cowden综合征的器官特异性和性别特异性瘤形成易感性,以及为什么只有一小部分具有生殖PTEN突变的女性会患上乳腺癌,取决于雄激素类固醇的环境和水平。

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