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Quantitative profiles of the mRNAs of ER-α and its novel variant ER-α36 in breast cancers and matched normal tissues

机译:乳腺癌和匹配的正常组织中ER-α及其新变异体ER-α36mRNA的定量特征

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摘要

Objective: The novel estrogen receptor-α (ER-α) variant ER-α36 is reported to be functional in the estrogen signaling pathway and is related to tamoxifen resistance in breast cancer. However, ER-α36 tends to be a favorable factor for survival in patients without tamoxifen therapy. To investigate the mechanisms behind this paradox, we determined the differences between the transcriptional profiles of ER-α36 and full-length ER-α (ER-α66) in breast cancers and matched normal tissues. Methods: We analyzed ER-α36 and ER-α66 messenger RNA (mRNA) levels in 74 pairs of breast cancers and matched normal tissues using a real-time quantitative polymerase chain reaction (PCR) assay, and correlated the results with their clinicopathological characteristics. Results: Breast cancers expressed lower ER-α36 mRNA levels than matched normal tissues regardless of their ER-α66 expression status. Down-regulation of ER-α36 mRNA was correlated with local progression, lymph node metastasis, and advanced cancer stage. The level of ER-α66 mRNA was lower in ER-α negative breast cancers compared with matched normal tissues. No differences in ER-α66 mRNA levels were observed during cancer progression. Conclusion: Down-regulation of ER-α36 is associated with carcinogenesis and progression of breast cancer.
机译:目的:据报道,新型雌激素受体-α(ER-α)变体ER-α36在雌激素信号通路中起作用,并且与乳腺癌中他莫昔芬的耐药性有关。但是,ER-α36往往是未经他莫昔芬治疗的患者生存的有利因素。为了研究这种悖论背后的机制,我们确定了乳腺癌和匹配的正常组织中ER-α36和全长ER-α(ER-α66)的转录谱之间的差异。方法:我们使用实时定量聚合酶链反应(PCR)分析了74对乳腺癌和匹配的正常组织中的ER-α36和ER-α66信使RNA(mRNA)水平,并将结果与​​它们的临床病理特征相关联。结果:乳腺癌的ER-α36mRNA水平低于匹配的正常组织,无论其ER-α66表达状态如何。 ER-α36mRNA的下调与局部进展,淋巴结转移和晚期癌症相关。与匹配的正常组织相比,ER-α阴性乳腺癌中的ER-α66mRNA水平较低。在癌症进展过程中未观察到ER-α66mRNA水平的差异。结论:ER-α36的下调与乳腺癌的发生和发展有关。

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