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Serial circulating tumor DNA identification associated with the efficacy and prognosis of neoadjuvant chemotherapy in breast cancer

机译:串行循环肿瘤DNA鉴定与乳腺癌新辅助化疗的疗效和预后相关

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Background Circulating tumor DNA (ctDNA) provides a promising noninvasive alternative to evaluate the efficacy of neoadjuvant chemotherapy (NCT) in breast cancer. Methods Herein, we collected 63 tissue (aspiration biopsies and resected tissues) and 206 blood samples (baseline, during chemotherapy (Chemo), after chemotherapy (Post-Chemo), after operation (Post-Op), during follow-up) from 32 patients, and preformed targeted deep sequencing with a customed 1021-gene panel. Results As the results, TP53 (43.8%) and PIK3CA (40.6%) were the most common mutant genes in the primary tumors. At least one tumor-derived mutation was detected in the following number of blood samples: 21, baseline; 3, Chemo; 9, Post-Chemo; and 5, Post-Op. Four patients with pathologic complete response had no tissue mutation in Chemo and Post-Chemo blood. Compared to patients with mutation-positive Chemo or Post-Chemo blood, the counterparts showed a superior primary tumor decrease (median, 86.5% versus 54.6%) and lymph involvement (median, 1 versus 3.5). All five patients with mutation-positive Post-Op developed distant metastases during follow-up, and the sensitivity of detecting clinically relapsed patients was 71.4% (5/7). The median DFS was 9.8 months for patients with mutation-positive Post-Op but not reached for the others (HR 23.53; 95% CI, 1.904-290.9; p < 0.0001). Conclusions Our study shows that sequential monitoring of blood ctDNA was an effective method for evaluating NCT efficacy and patient recurrence. Integrating ctDNA profiling into the management of LABC patients might improve clinical outcome.
机译:背景技术循环肿瘤DNA(CTDNA)提供了有希望的非侵入性替代方案,以评估Neoadjuvant化疗(NCT)在乳腺癌中的功效。本文方法,我们收集了63个组织(抽吸活检和切除组织)和206个血液样本(在化疗期间(化疗),化疗(后化疗)后,在32期间进行后续行动(后op)之后)患者,用预热的1021-基因面板预先形成靶向深序。结果作为结果,TP53(43.8%)和PIK3CA(40.6%)是主要肿瘤中最常见的突变基因。在下列血液样品中检测到至少一种肿瘤衍生的突变:21,基线; 3,化疗; 9,后化疗;和5,后op。四名病理完全反应患者在化疗和化疗后血液中没有组织突变。与突变阳性化疗或后化疗后血液患者相比,对应物显示出优异的原发性肿瘤减少(中位数,86.5%,54.6%)和淋巴及(中位数,1与3.5)。所有五名突变阳性患者患者在随访期间开发了远处转移,检测临床复发患者的敏感性为71.4%(5/7)。突变阳性后后患者的中位数DFS为9.8个月,但未达到其他患者(HR 23.53; 95%CI,1.904-290.9; P <0.0001)。结论我们的研究表明,血液CTDNA的顺序监测是评估NCT疗效和患者复发的有效方法。将CTDNA分析集成到Labc患者的管理中可能改善临床结果。

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