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Overexpression of eukaryotic initiation factor 4e is correlated with increased risk for systemic dissemination in node-positive breast cancer patients

机译:真核引发因子4e的过表达与节点阳性乳腺癌患者的全身散射风险增加相关

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Background Molecular events impact systemic dissemination. Overexpression of eukaryotic initiation factor 4E (eIF4E) has been shown to predict worse clinical outcomes in breast cancer. Node-positive breast cancer patients were specifically studied to determine if eIF4E elevation increases risk for systemic dissemination. Study design Two hundred two node-positive breast cancer patients were prospectively accrued and treated with standardized treatment and surveillance protocol. Tumor eIF4E protein level was quantified by Western blots as x-fold over benign samples from noncancer patients. Primary end point was systemic metastasis. Results Systemic recurrence was detected in 22.2% of the low eIF4E group, 27.3% of the intermediate group, and 49% of the high group, at a median follow-up of 47 months. A greater risk for systemic metastasis was seen in the high eIF4E group compared with the low group (log-rank test, p = 0.0084). Patients in the high eIF4E group had a 1.5-fold (hazard ratio = 1.52; 95% CI, 1.07-2.17; p = 0.0206) higher risk for systemic metastasis than the low group. Sixty percent of the patients with high eIF4E were observed to have metastasis to multiple sites, compared with 50% in the intermediate group, and 14.5% in the low group (p = 0.02, Fisher's exact test). When patients were segregated based on nodal classification (N1, N2, and N3), eIF4E overexpression continued to be a predictor for systemic dissemination in patients with N1 disease. Conclusions High eIF4E is correlated with an increased risk for systemic metastasis in node-positive breast cancer patients. High eIF4E overexpression was associated with a higher incidence of metastasis to multiple sites. Therefore, high eIF4E overexpression appears to be a marker for molecular events that increases risk for systemic dissemination.
机译:背景分子事件影响全身传播。已经显示了真核引发因子4e(EIF4E)的过表达预测乳腺癌中的临床结果较差。专门研究节点阳性乳腺癌患者,以确定EIF4E升高是否会增加系统传播的风险。研究设计两百节点阳性乳腺癌患者均经过正面累积和治疗标准化治疗和监测方案。肿瘤EIF4E蛋白质水平通过Western印迹量化为来自非癌症患者的良性样品的X型折叠。主要终点是全身转移。结果在低EIF4E组的22.2%,中间组的22.3%和49%的高组中,检测到全身复发,在47个月的中间随访中,49%。与低群体相比,高EIF4E组中可以在高EIF4E组中看到全身转移风险(对数级测试,P = 0.0084)。高EIF4E组中的患者具有1.5倍(危害比率= 1.52; 95%CI,1.07-2.17; P = 0.0206),其系统转移的风险较高,而不是低组织。 60%的高EIF4E患者被观察到多个位点转移,与中间组中的50%相比,低组织中14.5%(P = 0.02,Fisher的确切测试)。当基于节点分类(N1,N2和N3)进行患者进行分离时,EIF4E过表达仍然是N1疾病患者的全身散移的预测因子。结论高EIF4E与节点阳性乳腺癌患者的全身转移的风险增加。高EIF4E过表达与多个位点的转移发病率较高有关。因此,高EIF4E过表达似乎是用于增加全身传播风险的分子事件的标志物。

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    Department of Surgery Louisiana State University Health School of Medicine Feist-Weiller Cancer;

    Department of Surgery Louisiana State University Health School of Medicine Feist-Weiller Cancer;

    Department of Surgery Louisiana State University Health School of Medicine Feist-Weiller Cancer;

    Department of Surgery Louisiana State University Health School of Medicine Feist-Weiller Cancer;

    Department of Surgery Louisiana State University Health School of Medicine Feist-Weiller Cancer;

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