首页> 外文期刊>Annals of surgical oncology >Intense Expression of EGFR L858R Characterizes the Micropapillary Component and L858R Is Associated with the Risk of Recurrence in pN0M0 Lung Adenocarcinoma with the Micropapillary Component
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Intense Expression of EGFR L858R Characterizes the Micropapillary Component and L858R Is Associated with the Risk of Recurrence in pN0M0 Lung Adenocarcinoma with the Micropapillary Component

机译:EGFR L858R的强烈表达表征了微杂种组分,L858R与PN0M0肺腺癌的复发风险与微小足体部件相关联

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Background Lung adenocarcinoma with the micropapillary (MP) component poses a higher risk of recurrence even when the MP component is not predominant. This study explored genetic features associated with highly malignant behavior of lung adenocarcinoma with the MP component. Methods The MP and papillary (PaP) components were captured separately in three patients. Comprehensive mRNA expressions of somatic variants were compared between the MP and PaP components of each patient using next-generation sequencing (NGS). The protein expression of the NGS-detected variant was validated by immunohistochemistry. The prognostic impact of the detected variant was evaluated in 288 adenocarcinoma patients with resection of pN0M0. Results In two cases, NGS suggested higher RNA expression of EGFR L858R in the MP component than in the PaP component (allele frequency, 0.485 vs. 0.155 and 1.000 vs. 0.526, respectively; P < 0.001 for both). Immunohistochemistry validated intense expression of L858R in the MP component of 27 MP-positive (MP+) patients. Among 288 pN0M0 patients, L858R was more frequently harbored in the MP+ patients than in the MP-negative (MP-) patients. The MP+ patients harboring L858R showed significantly worse recurrence-free survival (RFS) than the MP+ patients without L858R (median RFS 38.7 and 55.0 months, respectively; hazard ratio [HR] 3.004; 95% confidence interval [CI] 1.306-9.132; P = 0.012). Multivariate analysis of the MP+ patients showed that positive L858R status was associated with poorer RFS (HR 2.976; 95% CI 1.190-7.442; P = 0.020). Conclusions EGFR L858R was more frequently harbored in the MP+ adenocarcinoma patients than in the MP- adenocarcinoma patients. Intense expression of L858R in the MP component was suggested, and the MP+ patients harboring L858R were at comparatively higher risk of recurrence in the group with pN0M0 lung adenocarcinoma.
机译:背景技术即使当MP组分不是主要的时,肺腺癌与微小足体(MP)分量的血糖腺癌造成更高的复发风险。本研究探讨了与MP组分肺腺癌的高度恶性行为相关的遗传特征。方法在三名患者中单独捕获MP和乳头状(PAP)组分。使用下一代测序(NGS)比较每位患者的MP和PAP组分之间进行体躯体变体的综合mRNA表达。通过免疫组织化学验证了NGS检测变体的蛋白质表达。检测到的变异的预后局部在288例腺癌患者中评估了PN0M0的切除术。结果在两种情况下,NGS在MP组分中提出了EGFR L858R的更高RNA表达,而不是PAP组分(等位基因频率,0.485与0.155和1.000 vs.0.526).P <0.001两个)。免疫组织化学在27MP阳性(MP +)患者的MP分量中L858R的敏感表达。在288例PN0M0患者中,在MP +患者中,L858R更常见于MP +患者,而不是在MP阴性(MP-)患者中。患有L858R的MP +患者显着越差,不含L858R的MP +患者(分别为38.7和55.0个月的中位数;危害比[HR] 3.004; 95%置信区间[CI] 1.306-9.132; P. = 0.012)。 MP +患者的多变量分析表明,阳性L858R状态与较差的RFS相关(HR 2.976; 95%CI 1.190-7.442; P = 0.020)。结论EGFR L858R在MP +腺癌患者中更常见于MP-腺癌患者。提出了L858R在MP组分中的强烈表达,患有L858R的MP +患者在具有PN0M0肺腺癌的组中复发的相对较高的风险。

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