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首页> 外文期刊>AIDS Research and Human Retroviruses >Female Sex Hormones Activate Human Endogenous Retrovirus Type K Through the OCT4 Transcription Factor in T47D Breast Cancer Cells
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Female Sex Hormones Activate Human Endogenous Retrovirus Type K Through the OCT4 Transcription Factor in T47D Breast Cancer Cells

机译:女性性激素通过T47D乳腺癌细胞的OCT4转录因子激活人内源性逆转录病毒K

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摘要

Female sex hormones, the octamer-binding transcription factor 4 (OCT4), and human endogenous retroviruses (HERVs) are all involved in the development of breast cancer. However, whether there are cross talks between these factors to promote breast cancer is still unknown. Using the T47D human breast cancer cell line, we have found that estradiol and progesterone synergistically activate HERV-K through nuclear receptors. The progesterone receptor (isoform B) binds a progesterone-response element (PRE) in a long terminal repeat (LTR5HS) of HERV-K. There is another transcription factor-binding element in the LTR, the octamer motif, which is required for the hormones to activate gene transcription downstream of the LTR. Gel shift assays and co-immunoprecipitation indicate that the progesterone receptor (PR) and the OCT4 transcription factor interact on the protein level. Methylation of the PRE enhances binding of the PR. These findings help to elucidate the previously unknown cross talks among the sex hormones, OCT4, and HERVs in contributing to breast cancer proliferation and tumorigenesis, which may be useful in guiding further development of cancer therapies.
机译:女性性激素,八胞胎结合转录因子4(Oct4)和人内源性逆转录病毒(Hervs)都参与了乳腺癌的发育。但是,在这些因素之间是否有跨谈促进乳腺癌仍然未知。使用T47D人乳腺癌细胞系,我们发现雌二醇和黄体酮通过核受体协同激活肝病患者。孕酮受体(同种型B)结合HERV-K的长末端重复(LTR5HS)中的孕激素响应元件(PRE)。在LTR中存在另一种转录因子结合元件,八氧酮基质是激素所必需的,激素激活LTR下游的基因转录。凝胶移位测定和共免疫沉淀表明孕酮受体(PR)和OCT4转录因子对蛋白质水平相互作用。预增强了PR的结合的甲基化。这些发现有助于阐明性激素,Oct4和患者之间的先前未知的交叉谈判,以促进乳腺癌增殖和肿瘤发生,这可能有助于引导癌症治疗的进一步发展。

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