The prognosis and adjuvant chemotherapy in KRAS mutation patients with stage I lung adenocarcinoma

Clinical Surgical Oncology Pub Date : 2024-12-01 DOI:10.1016/j.cson.2024.100069

Shangshang Ma , Kun Li , Rangrang Wang , Jiayi Qian , Yongfei Fan , Xichun Qin , Mingjun Li , Leilei Wu

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Abstract

Background

Adjuvant chemotherapy (ACT) remains the current first-line systemic treatment option for patients with KRAS-mutated lung adenocarcinoma (LUAD), but the response is not effective. The prognosis of ACT in patients with KRAS mutations in stage I LUAD has not yet been effectively explored.

Methods

Detailed data about patients with stage I LUAD from Shanghai Pulmonary Hospital were collected in this ambispective study. Pearson's Chi-square test, Kaplan-Meier analysis, and Cox proportional hazard models were performed in this study. The primary observational endpoint was overall survival (OS). Sensitivity analysis was performed to assess the robustness of the findings.

Results

In this study population, 10.87% (194 out of 1783) of stage I LUAD patients possessed KRAS mutations. In the KRAS-mutated cohort, 7 patients harbored EGFR L858R point mutation, 2 patients exhibited EGFR exon 19 Del mutation, 2 patients had ALK rearrangement, and 1 patient for other EGFR mutations. Patients harboring KRAS mutations had a worse OS compared to KRAS wild-type (WT) patients (5-year OS rate: 96% vs. 82%, P < 0.001). In addition, the KARS(G12C) mutation was an independent factor for poor prognosis (P < 0.001). Importantly, ACT improved survival in patients with stage IB LUAD (P = 0.02) while not improved survival in the group of stage IB patients with KRAS mutations (P = 0.31).

Conclusions

KRAS mutation could co-occur with EGFR mutation and ALK rearrangement. KRAS mutation was associated with poor prognosis in stage I LUAD patients. In addition, ACT did not improve prognosis in stage IB LUAD patients with KRAS mutations. Our findings require more research to be confirmed.

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KRAS突变I期肺腺癌患者的预后及辅助化疗

背景：辅助化疗（ACT）仍然是目前kras突变肺腺癌（LUAD）患者的一线全身治疗选择，但反应并不有效。对于KRAS突变的I期LUAD患者，ACT的预后尚未得到有效探讨。方法收集上海市肺科医院I期LUAD患者的详细资料。本研究采用Pearson卡方检验、Kaplan-Meier分析和Cox比例风险模型。主要观察终点是总生存期（OS）。进行敏感性分析以评估研究结果的稳健性。结果在本研究人群中，1783例I期LUAD患者中有194例（10.87%）具有KRAS突变。在kras突变队列中，7例患者存在EGFR L858R点突变，2例患者存在EGFR外显子19 Del突变，2例患者存在ALK重排，1例患者存在其他EGFR突变。与KRAS野生型（WT）患者相比，携带KRAS突变的患者的OS更差(5年OS率：96% vs 82%， P <；0.001)。此外，KARS（G12C）突变是预后不良的独立因素(P <；0.001)。重要的是，ACT提高了IB期LUAD患者的生存率（P = 0.02），而IB期KRAS突变患者的生存率没有提高（P = 0.31）。结论skras突变可能与EGFR突变和ALK重排同时发生。KRAS突变与I期LUAD患者预后不良相关。此外，ACT并没有改善IB期LUAD患者KRAS突变的预后。我们的发现需要更多的研究来证实。

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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Clinical Surgical Oncology

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