Prognostic impact of targetable driver alterations in resected early-stage lung cancer.

IF 4 2区医学 Q2 ONCOLOGY Translational lung cancer research Pub Date : 2024-11-30 Epub Date: 2024-11-14 DOI:10.21037/tlcr-24-433

Angelika Terbuch, Selma Konjic, Verena Schlintl, Gudrun Absenger, Philipp J Jost, Jörg Lindenmann, Paul Swatek, Nikolaus John, Teresa John, Robert Wurm, Martin Zacharias, Florian Posch, Maximilian J Hochmair, Hannah Fabikan, Christoph Weinlinger, Oliver Illini, Lena Horvath, Gabriele Gamerith, Dominik Wolf, Florian Augustin, Luka Brcic

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Abstract

Background: Apart from ALK fusions and the common EGFR mutations, targetable molecular alterations are irrelevant for adjuvant treatment decision making in early-stage non-small cell lung cancer (NSCLC). This retrospective analysis aimed to investigate if there is a difference in recurrence-free survival in stage I-III NSCLC harboring druggable molecular alterations compared to subtypes without targetable molecular alterations.

Methods: All consecutive patients who underwent surgery with curative intent for NSCLC (stage I-III) with targetable mutations between January 2015 and December 2020 at three Austrian institutions were identified and compared with tumors without targetable molecular alterations. Tumors with the EGFR-mutated subtype were excluded due to already existing results from prospective trials.

Results: One hundred and sixty subjects had tumors with molecular alterations and 355 subjects served as control cohort. There was a higher prevalence of female sex (P<0.001) and never-smokers (P=0.01) among patients with tumors harboring oncogenic driver mutations. The three most common alterations were the KRAS G12C mutation (n=92), ALK fusions (n=21), and the BRAF V600E mutation (n=15). The 1-, 3- and 5-year cumulative incidence of recurrence estimates were 16%, 38% and 46% in patients without molecular alterations and 16%, 38% and 48% in patients with the KRAS G12C mutation and 12%, 33% and 55% in patients with other molecular alterations, respectively (P=0.89). Univariable predictors of an increased recurrence risk were higher tumor stage (P<0.001), receipt of neoadjuvant treatment (P<0.001) and receipt of adjuvant treatment (P=0.03). The lack of association between molecular alteration status and recurrence risk prevailed after multivariable adjustment for tumor stage and perioperative treatment (P=0.82 for KRAS G12C mutation and P=0.43 for any other molecular alteration).

Conclusions: NSCLC patients with resected tumors that harbor molecular alterations have the same recurrence risk as patients with tumors without molecular alterations if treated with surgery plus chemotherapy when indicated.

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切除的早期肺癌中可靶向驱动改变对预后的影响。

背景：除了ALK融合和常见的EGFR突变外，可靶向的分子改变与早期非小细胞肺癌（NSCLC）的辅助治疗决策无关。本回顾性分析旨在研究I-III期NSCLC中具有可药物分子改变的患者与无靶向分子改变的亚型患者的无复发生存率是否存在差异。方法：在2015年1月至2020年12月期间，在奥地利的三家机构中，所有连续接受手术治疗的具有靶向突变的NSCLC （I-III期）患者被确定并与无靶向分子改变的肿瘤进行比较。由于前瞻性试验的现有结果，egfr突变亚型的肿瘤被排除在外。结果：肿瘤分子改变者160例，对照组355例。女性患病率较高(PKRAS G12C突变（n=92）、ALK融合（n=21）和BRAF V600E突变（n=15）。无分子改变患者的1、3和5年累积复发率分别为16%、38%和46%，KRAS G12C突变患者的1、3和5年累积复发率分别为16%、38%和48%，其他分子改变患者的1、3和5年累积复发率分别为12%、33%和55% （P=0.89）。增加复发风险的单变量预测因子是更高的肿瘤分期（PKRAS G12C突变，其他任何分子改变P=0.43）。结论：切除肿瘤并伴有分子改变的非小细胞肺癌患者与未发生分子改变的肿瘤患者如果在需要时进行手术加化疗，其复发风险相同。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Translational lung cancer research Medicine-Oncology

CiteScore

7.20

自引率

2.50%

发文量

137

期刊介绍： Translational Lung Cancer Research(TLCR, Transl Lung Cancer Res, Print ISSN 2218-6751; Online ISSN 2226-4477) is an international, peer-reviewed, open-access journal, which was founded in March 2012. TLCR is indexed by PubMed/PubMed Central and the Chemical Abstracts Service (CAS) Databases. It is published quarterly the first year, and published bimonthly since February 2013. It provides practical up-to-date information on prevention, early detection, diagnosis, and treatment of lung cancer. Specific areas of its interest include, but not limited to, multimodality therapy, markers, imaging, tumor biology, pathology, chemoprevention, and technical advances related to lung cancer.