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Combined HER3-EGFR score in triple-negative breast cancer provides prognostic and predictive significance superior to individual biomarkers

机译:三重阴性乳腺癌中的Her3-EGFR评分提供了高于个体生物标志物的预后和预测意义

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Epidermal growth factor receptor (EGFR) and human epidermal growth factor receptor 3 (HER3) have been investigated as triple-negative breast cancer (TNBC) biomarkers. Reduced EGFR levels can be compensated by increases in HER3; thus, assaying EGFR and HER3 together may improve prognostic value. In a multi-institutional cohort of 510 TNBC patients, we analyzed the impact of HER3, EGFR, or combined HER3-EGFR protein expression in pre-treatment samples on breast cancer-specific and distant metastasis-free survival (BCSS and DMFS, respectively). A subset of 60 TNBC samples were RNA-sequenced using massive parallel sequencing. The combined HER3-EGFR score outperformed individual HER3 and EGFR scores, with high HER3-EGFR score independently predicting worse BCSS (Hazard Ratio [HR]?=?2.30, p?=?0.006) and DMFS (HR?=?1.78, p?=?0.041, respectively). TNBCs with high HER3-EGFR scores exhibited significantly suppressed ATM signaling and differential expression of a network predicted to be controlled by low TXN activity, resulting in activation of EGFR, PARP1, and caspases and inhibition of p53 and NFκB. Nuclear PARP1 protein levels were higher in HER3-EGFR-high TNBCs based on immunohistochemistry (p?=?0.036). Assessing HER3 and EGFR protein expression in combination may identify which adjuvant chemotherapy-treated TNBC patients have a higher risk of treatment resistance and may benefit from a dual HER3-EGFR inhibitor and a PARP1 inhibitor.
机译:表皮生长因子受体(EGFR)和人表皮生长因子受体3(HER3)已被研究为三阴性乳腺癌(TNBC)生物标志物。减少的EGFR水平可以通过HER3的增加来补偿;因此,分析EGFR和HER3可以改善预后值。在510例TNBC患者的多机构队列中,我们分析了HER3,EGFR或组合HER3-EGFR蛋白表达在乳腺癌特异性和远处转移存活中的预处理样品中的影响(分别分别是BCS和DMF) 。使用大规模平行测序的60 TNBC样品的子集是RNA测序。 HER3-EGFR分数表现优于个体HER3和EGFR分数,高HER3-EGFR评分独立预测更差的BCS(危险比[HR]?=?2.30,P?0.006)和DMFS(HR?=?1.78,P ?=?0.041分别)。具有高HER3-EGFR评分的TNBCS表现出显着抑制的ATM信号传导和预测由低TXN活性控制的网络的差异表达,导致EGFR,PARP1和半胱天冬酶的激活和P53和NFκB的抑制。 HER3-EGFR-HIGHT TNBCS的核PARP1蛋白水平基于免疫组织化学(P?= 0.036)。评估HER3和EGFR蛋白表达组合可以鉴定哪种佐剂化疗处理的TNBC患者具有更高的治疗风险,并且可以从双HER3-EGFR抑制剂和PARP1抑制剂中受益。

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