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首页> 外文期刊>Journal of Thoracic Disease >Circulating free tumor-derived DNA to detect EGFR mutations in patients with advanced NSCLC: French subset analysis of the ASSESS study
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Circulating free tumor-derived DNA to detect EGFR mutations in patients with advanced NSCLC: French subset analysis of the ASSESS study

机译:循环游离肿瘤来源的DNA检测晚期NSCLC患者的EGFR突变:ASSESS研究的法国子集分析

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Background: The non-interventional ASSESS study (NCT01785888) evaluated the utility of circulating free tumor-derived DNA (ctDNA) from plasma for epidermal growth factor receptor ( EGFR ) mutation testing in patients with advanced non-small-cell lung cancer (NSCLC), in a real-world setting across 56 centers in Europe and Japan. The high mutation status concordance between 1162 matched tissue/cytology and plasma samples (89%, sensitivity =46%, specificity =97%) suggested that ctDNA is a feasible sample for EGFR mutation analysis. We report data for the French subset of patients (pre-planned analysis). Methods: Eligible patients (stage IIIA/B/IV locally advanced/metastatic treatment-naive advanced NSCLC) provided diagnostic tissue/cytology and plasma samples. DNA extracted from tissue/cytology samples was subjected to EGFR mutation testing as per local practice; a designated laboratory performed ctDNA extraction/mutation testing of plasma samples. The primary outcome was EGFR mutation status concordance between matched tumor and plasma samples. Results: Of the 1,311 patients enrolled in the ASSESS trial, 145 were recruited from 9 centers in France. Tumor samples from 130 patients were collected and 126 were evaluable for EGFR mutation analysis. Activating EGFR mutations were identified in 13 of the 126 patient tumor samples ( EGFR mutation frequency 10.3%). For plasma testing, 10 of the 145 samples tested were positive for EGFR mutations ( EGFR mutation frequency 6.9%). EGFR mutation rate was significantly higher in never- versus ever-smokers (stepwise logistic regression: tumor, P0.0001; plasma, P=0.0008). Mutation status concordance between 126 matched patient samples was 96.0% [121/126; 95% confidence intervals (CI), 91.0–98.7]. Of the 113 EGFR mutation-negative patient tissue samples, one tested plasma-positive; reanalysis of plasma via two different techniques confirmed the presence of a L858R mutation, indicating a tissue false-negative result. Based on these data, sensitivity of plasma testing was 64.3% (9/14; 95% CI, 35.1–87.2%) and its specificity was 100.0% (112/112; 95% CI, 96.8–100.0%). Conclusions: Data confirm ctDNA as an alternative sample for EGFR mutation analysis in patients with advanced NSCLC.
机译:背景:非介入性研究(NCT01785888)评估了血浆中游离游离肿瘤衍生DNA(ctDNA)在晚期非小细胞肺癌(NSCLC)患者中用于表皮生长因子受体(EGFR)突变测试的实用性,在现实世界中遍及欧洲和日本的56个中心。在1162个匹配的组织/细胞学与血浆样品之间的高度突变状态一致性(89%,灵敏度= 46%,特异性= 97%)表明,ctDNA是用于EGFR突变分析的可行样品。我们报告法国患者子集的数据(预先计划的分析)。方法:符合条件的患者(IIIA / B / IV期局部晚期/转移治疗-未治疗的晚期NSCLC)提供了诊断性组织/细胞学和血浆样本。从组织/细胞学样本中提取的DNA按照当地惯例进行EGFR突变测试;指定实验室对血浆样品进行了ctDNA提取/突变测试。主要结果是匹配的肿瘤和血浆样品之间的EGFR突变状态一致性。结果:参加ASSESS试验的1,311名患者中,有145名是从法国9个中心招募的。收集了130例患者的肿瘤样本,并对126个样本进行了EGFR突变分析。在126例患者肿瘤样本中的13个中鉴定出了激活的EGFR突变(EGFR突变频率为10.3%)。对于血浆测试,在145个样本中,有10个样本的EGFR突变为阳性(EGFR突变频率为6.9%)。从不吸烟者和从未吸烟者的EGFR突变率显着更高(逐步逻辑回归:肿瘤,P <0.0001;血浆,P = 0.0008)。 126个匹配的患者样本之间的突变状态一致性为96.0%[121/126; 95%置信区间(CI),91.0–98.7]。在113例EGFR突变阴性的患者组织样本中,有1例血浆阳性。通过两种不同的技术对血浆进行的重新分析证实了L858R突变的存在,表明组织假阴性结果。根据这些数据,血浆测试的敏感性为64.3%(9/14; 95%CI,35.1–87.2%),其特异性为100.0%(112/112; 95%CI,96.8-100.0%)。结论:数据证实ctDNA是晚期NSCLC患者EGFR突变分析的替代样品。

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