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首页> 外文期刊>Breast cancer research and treatment. >Expression of PEA3 and lack of correlation between PEA3 and HER-2eu expression in breast cancer.
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Expression of PEA3 and lack of correlation between PEA3 and HER-2eu expression in breast cancer.

机译:乳腺癌中PEA3的表达以及PEA3和HER-2 / neu表达之间没有相关性。

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摘要

The ETS protein PEA3 functions as a transcription factor to regulate gene expression. Although members of the ETS family have been reported to be involved in tumor progression, ectopic expression of PEA3 has been shown to suppress tumor formation. Despite several studies demonstrated frequent expression of PEA3 and its high association with HER-2eu and have suggested a potential role of PEA3 in breast cancer, contradictory result has shown that the PEA3 was associated with better survival rate in breast cancer. In the current study, we address this discrepancy by examining the expression of PEA3 and HER-2eu on 289 archived breast cancer tumor tissues and their correlation with clinicopathologic factors and prognosis. The staining of PEA3 was further validated by in situ hybridization for PEA3 mRNA. We found PEA3 was positive in 22.2% (64/289) of all cases and only 25.6% (21/82) of HER-2eu-overexpressing cases showed co-expression of PEA3. In contrast to HER-2eu, PEA3 expression was not correlated with prognosis or major clinicopathologic factors, except for a negative correlation with lymphovascular permeation ( p=0.007). This study demonstrates that PEA3 expression is not correlated with HER-2eu expression in breast cancer tumor tissues, nor is it associated with adverse clinicopathologic factors or prognosis.
机译:ETS蛋白PEA3作为转录因子来调节基因表达。尽管已经报道了ETS家族的成员参与肿瘤的进展,但是PEA3的异位表达已显示出抑制了肿瘤的形成。尽管有几项研究表明PEA3的频繁表达及其与HER-2 / neu的高度关联,并暗示了PEA3在乳腺癌中的潜在作用,但矛盾的结果表明,PEA3与乳腺癌的更高生存率相关。在当前的研究中,我们通过检查289个已存档的乳腺癌肿瘤组织中PEA3和HER-2 / neu的表达及其与临床病理因素和预后的相关性来解决这一差异。通过PEA3 mRNA的原位杂交进一步验证了PEA3的染色。我们发现在所有病例中,PEA3阳性的占22.2%(64/289),而在HER-2 / neu过表达的病例中只有25.6%(21/82)表现出PEA3的共表达。与HER-2 / neu相比,PEA3的表达与预后或主要的临床病理因素无关,除了与淋巴管渗透性呈负相关(p = 0.007)。这项研究表明,PEA3表达与乳腺癌肿瘤组织中的HER-2 / neu表达无关,也与不良的临床病理因素或预后无关。

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