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A PAM50-based chemoendocrine score for hormone receptor-positive breast cancer with an intermediate risk of relapse

机译:基于pam50的激素受体阳性乳腺癌化学内分泌评分,具有中度复发风险

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摘要

Purpose: Hormone receptor-positive (HR+) breast cancer is clinically and biologically heterogeneous, and subgroups with different prognostic and treatment sensitivities need to be identified.Experimental Design: Research-based PAM50 subtyping and expression of additional genes was performed on 63 patients with HR+/HER2- disease randomly assigned to neoadjuvant multiagent chemotherapy versus endocrine therapy in a phase II trial. The biology associated with treatment response was used to derive a PAM50-based chemoendocrine score (CES). CES's predictive ability was evaluated in 4 independent neoadjuvant data sets (n = 675) and 4 adjuvant data sets (n = 1,505). The association of CES, intrinsic biology, and PAM50 risk of relapse (ROR) was explored across 6,007 tumors.Results: Most genes associated with endocrine sensitivity were also found associated with chemotherapy resistance. In the chemotherapy test/validation data sets, CES was independently associated with pathologic complete response (pCR), even after adjusting for intrinsic subtype. pCR rates of the CES endocrine-sensitive (CES-E), uncertain (CES-U), and chemotherapy-sensitive (CES-C) groups in both data sets combined were 25%, 11%, and 2%, respectively. In the endocrine test/validation data sets, CES was independently associated with response. Compared with ROR, >90% of ROR-low and ROR-high tumors were identified as CES-E and CES-C, respectively; however, each CES group represented >25% of ROR-intermediate disease. In terms of survival outcome, CES-C was associated with poor relapse-free survival in patients with ROR-intermediate disease treated with either adjuvant endocrine therapy only or no adjuvant systemic therapy, but not in patients treated with (neo)adjuvant chemotherapy.Conclusions: CES is a genomic signature capable of estimating chemoendocrine sensitivity in HR+ breast cancer beyond intrinsic subtype and risk of relapse
机译:目的:激素受体阳性(HR +)乳腺癌在临床和生物学上是异质性的,需要确定具有不同预后和治疗敏感性的亚组实验设计:对63例HR +患者进行了基于研究的PAM50亚型和其他基因的表达II期试验将/ HER2-疾病随机分配给新辅助多药化疗与内分泌治疗。与治疗反应相关的生物学用于得出基于PAM50的化学内分泌评分(CES)。在4个独立的新辅助数据集(n = 675)和4个辅助数据集(n = 1,505)中评估了CES的预测能力。研究人员在6,007个肿瘤中探讨了CES,内在生物学和PAM50复发风险(ROR)的关系。结果:大多数与内分泌敏感性相关的基因也被发现与化疗耐药有关。在化学疗法测试/验证数据集中,即使在调整固有亚型后,CES也独立与病理完全缓解(pCR)相关。两种数据集的CES内分泌敏感(CES-E)组,不确定(CES-U)和化疗敏感(CES-C)组的pCR率分别为25%,11%和2%。在内分泌测试/验证数据集中,CES与反应独立相关。与ROR相比,分别有> 90%的ROR低和ROR高的肿瘤被鉴定为CES-E和CES-C。但是,每个CES组代表了ROR中级疾病的25%以上。就生存结局而言,仅接受辅助内分泌治疗或不接受辅助全身治疗的ROR中度疾病患者,CES-C与无复发生存率差相关,但接受(新)辅助化学治疗的患者则无此相关性。 :CES是一种基因组学特征,能够评估HR +乳腺癌对内分泌亚型和复发风险的化学内分泌敏感性

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    Prat, Aleix; Alba, Emilio;

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  • 年度 2017
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  • 正文语种 eng
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