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Proteomics profiling identify CAPS as a potential predictive marker of tamoxifen resistance in estrogen receptor positive breast cancer

机译:蛋白质组学分析确定CAPS是雌激素受体阳性乳腺癌中他莫昔芬耐药性的潜在预测指标

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摘要

BACKGROUND: Despite the success of tamoxifen since its introduction, about one-third of patients with estrogen (ER) and/or progesterone receptor (PgR) - positive breast cancer (BC) do not benefit from therapy. Here, we aim to identify molecular mechanisms and protein biomarkers involved in tamoxifen resistance. RESULTS: Using iTRAQ and Immobilized pH gradient-isoelectric focusing (IPG-IEF) mass spectrometry based proteomics we compared tumors from 12 patients with early relapses (<2 years) and 12 responsive to therapy (relapse-free > 7 years). A panel of 13 proteins (TCEAL4, AZGP1, S100A10, ALDH6A1, AHNAK, FBP1, S100A4, HSP90AB1, PDXK, GFPT1, RAB21, MX1, CAPS) from the 3101 identified proteins, potentially separate relapse from non-relapse BC patients. The proteins in the panel are involved in processes such as calcium (Ca(2+)) signaling, metabolism, epithelial mesenchymal transition (EMT), metastasis and invasion. Validation of the highest expressed proteins in the relapse group identify high tumor levels of CAPS as predictive of tamoxifen response in a patient cohort receiving tamoxifen as only adjuvant therapy. CONCLUSIONS: This data implicate CAPS in tamoxifen resistance and as a potential predictive marker.
机译:背景:尽管他莫昔芬自引入以来已获得成功,但约有三分之一患有雌激素(ER)和/或孕激素受体(PgR)-阳性乳腺癌(BC)的患者无法从治疗中受益。在这里,我们旨在确定与他莫昔芬抗性有关的分子机制和蛋白质生物标记。结果:使用iTRAQ和基于固定化pH梯度-等电聚焦(IPG-IEF)质谱的蛋白质组学,我们比较了12例早期复发(<2年)和12例对治疗敏感(无复发>> 7年)的肿瘤。来自3101种已鉴定蛋白的13种蛋白(TCEAL4,AZGP1,S100A10,ALDH6A1,AHNAK,FBP1,S100A4,HSP90AB1,PDXK,GFPT1,RAB21,MX1,CAPS)组成一组,可能将复发与非复发BC患者分开。专家组中的蛋白质参与诸如钙(Ca(2+))信号传导,代谢,上皮间质转化(EMT),转移和侵袭的过程。复发组中表达最高的蛋白质的验证确定,在接受他莫昔芬作为唯一辅助治疗的患者队列中,CAPS的高肿瘤水平预示了他莫昔芬反应。结论:该数据暗示CAPS对他莫昔芬有抗药性,并可能作为潜在的预测指标。

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