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Total Survivin and acetylated Survivin correlate with distinct molecular subtypes of breast cancer

机译:总生存素和乙酰化生存素与乳腺癌的不同分子亚型相关

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Global gene expression profiling studies led to the recent classification of breast cancer into 4 distinct molecular subtypes including luminal, human epidermal growth factor receptor 2 enriched, basal like, and unclassified. Here, we used immunohistochemistry to evaluate expression of the antiapoptotic protein Survivin and its recently described acetylated form, Survivin acetyl129, in normal breast tissue and in 226 primary breast tumors of different molecular subtypes. Correlation of Survivin expression with molecular markers and its impact on patient outcomes were analyzed. Eighty-four percent of basal-like tumors expressed high levels of total Survivin, whereas 52% of luminal tumors expressed high levels of acetylated Survivin (P <.001). Overall survival (91%) for tumors expressing low levels of total Survivin was better than that for tumors expressing high levels of total Survivin (72%, P =.02), whereas the reverse was true for tumors expressing acetylated Survivin. In hierarchical cluster analysis, total Survivin clustered with basal marker expression, whereas acetylated Survivin clustered with luminal marker expression. In multivariate analysis, high total Survivin expression was an independent predictor of worse overall survival in patients with breast cancer (relative risk, 11; P <.01). These data indicate that high levels of total Survivin predict poor outcome in patients with grade 3 invasive ductal carcinoma and correlate directly with a basal-like phenotype. In contrast, high expression of the acetylated form of the protein associates with a favorable outcome and preferentially correlates with luminal-type tumors. Survivin likely has different functions in distinct breast cancer subtypes, and diagnostic strategies that incorporate immunohistochemical markers that detect both Survivin forms may help better strategize patient risk and direct therapy.
机译:全球基因表达谱研究导致近期将乳腺癌分类为4种不同的分子亚型,包括腔内,人类表皮生长因子受体2富集,基底样和未分类。在这里,我们使用免疫组织化学评估抗凋亡蛋白Survivin及其最近描述的乙酰化形式Survivin acetyl129在正常乳腺组织和226种不同分子亚型的原发性乳腺肿瘤中的表达。分析了Survivin表达与分子标记的相关性及其对患者预后的影响。 84%的基底样肿瘤表达高水平的总Survivin,而52%的管腔肿瘤表达高水平的乙酰化Survivin(P <.001)。表达低水平总生存素的肿瘤的总生存率(91%)优于表达高水平总生存素的肿瘤的总生存率(72%,P = .02),而表达乙酰化生存素的肿瘤则相反。在层次聚类分析中,总的Survivin与基础标志物表达聚在一起,而乙酰化的Survivin与腔内标志物表达聚在一起。在多变量分析中,高的总生存素表达是乳腺癌患者总生存期较差的独立预测因子(相对风险,11; P <.01)。这些数据表明,高水平的总生存素预测患有3级浸润性导管癌的患者预后较差,并且与基底样表型直接相关。相反,蛋白质的乙酰化形式的高表达伴随着良好的结果,并优先与腔型肿瘤相关。 Survivin在不同的乳腺癌亚型中可能具有不同的功能,并且结合免疫组织化学标记物检测两种Survivin形式的诊断策略可能有助于更好地制定患者风险和直接治疗策略。

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