表皮生长因子受体驱动基因突变对新辅助放化疗和根治性手术后可切除局部晚期非小细胞肺癌病理完全缓解的影响。
Effects of EGFR driver mutations on pathologic regression in resectable locally advanced non-small cell lung cancer treated with neoadjuvant chemoradiation and completion surgery.
机构信息
Department of Radiation Oncology, Chaim Sheba Medical Center, Tel- Hashomer, Israel.
Department of Medical Oncology, Chaim Sheba Medical Center, Tel-Hashomer, Israel.
出版信息
Br J Radiol. 2023 Dec;96(1152):20220763. doi: 10.1259/bjr.20220763. Epub 2023 Oct 24.
OBJECTIVE
We hypothesized that driver mutations in epidermal growth factor receptor (EGFR) are associated with decreased pathologic response to neoadjuvant chemoradiation (NA-ChRT) in locally advanced non-small cell lung cancer (LA-NSCLC).
METHODS
Patients with Stage IIB-IIIA NSCLC treated with NA-ChRT, completion surgery, and underwent molecular profile testing were identified in a lung cancer database. Pathologic response was quantified using: (i) major pathologic response (MPR), (ii) complete pathologic response (pCR), and (iii) mean residual viable tumor cells (MRTC). Two groups were formed based on the presence or absence of driver mutations. Clinical and pathological correlations between the groups were studied.
RESULTS
Forty-seven patients underwent tumor molecular profile testing, NA-ChRT, and completion surgery. Compared to the no-driver mutation group, the driver mutation group had lower MPR (23% 71%, = 0.003), pCR (0% 26%, = 0.02), and higher MRTC (43.4% 15.8%, = 0.009). Univariate analysis showed an increased MPR rate for smokers, squamous cell histology, ChRT-surgery interval >65 days, and no-driver mutations. Multivariate analysis showed that only no-driver mutations (OR 0.39, = 0.02) remained significant for MPR. PD-L1 status did not affect MPR. At 2 years, the driver mutation group had lower rates of local control (Hazard ration [HR] 0.67, = 0.17) and disease-free survival (HR 0.5, = 0.001). Overall survival was similar for both groups (HR = 1.04, = 0.86).
CONCLUSION
Following 60 Gray NA-ChRT, tumors with a driver mutation had lower MPR and pCR rates than tumors without a driver mutation. PD-L1 was not associated with tumor regression.
ADVANCES IN KNOWLEDGE
Patients with resectable LA-NSCLC and an EGFR driver mutation treated with neoadjuvant-ChRT and completion surgery have reduced pathologic regression, lower local control rates, and shorter disease-free survival than patients without a driver mutation. Evaluation of molecular testing should be introduced in LA-NSCLC intended for prognostication and treatment decisions.
目的
我们假设表皮生长因子受体(EGFR)的驱动突变与局部晚期非小细胞肺癌(LA-NSCLC)新辅助放化疗(NA-ChRT)后的病理反应降低有关。
方法
在肺癌数据库中确定了接受 NA-ChRT、完成手术并进行分子谱检测的 IIB-IIIA 期 NSCLC 患者。使用以下方法量化病理反应:(i)主要病理反应(MPR),(ii)完全病理反应(pCR)和(iii)平均残留活肿瘤细胞(MRTC)。根据是否存在驱动突变将患者分为两组。研究两组之间的临床和病理相关性。
结果
47 名患者接受了肿瘤分子谱检测、NA-ChRT 和完成手术。与无驱动突变组相比,驱动突变组的 MPR(23%[71%], = 0.003)、pCR(0%[26%], = 0.02)和更高的 MRTC(43.4%[15.8%], = 0.009)较低。单因素分析显示,吸烟者、鳞状细胞组织学、ChRT-手术间隔>65 天和无驱动突变与 MPR 率增加有关。多因素分析显示,只有无驱动突变(OR 0.39, = 0.02)对 MPR 仍有显著影响。PD-L1 状态不影响 MPR。2 年时,驱动突变组的局部控制率(危险比 [HR] 0.67, = 0.17)和无病生存率(HR 0.5, = 0.001)较低。两组的总生存率相似(HR = 1.04, = 0.86)。
结论
接受 60 戈瑞 NA-ChRT 治疗后,具有驱动突变的肿瘤的 MPR 和 pCR 率低于无驱动突变的肿瘤。PD-L1 与肿瘤消退无关。
知识进展
接受新辅助-ChRT 和完成手术治疗的可切除局部晚期 NSCLC 且存在 EGFR 驱动突变的患者,其病理缓解程度降低,局部控制率降低,无病生存率缩短,与无驱动突变的患者相比。应在拟进行预后和治疗决策的 LA-NSCLC 中引入分子检测评估。
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