Prognostic Value of KRAS/TP53 Status for Overall Survival in First-Line Monoimmunotherapy and Chemoimmunotherapy Treated Patients With Nonsquamous NSCLC in the Netherlands: A Brief Report

IF 3 Q2 ONCOLOGY

JTO Clinical and Research Reports Pub Date : 2024-10-17 DOI:10.1016/j.jtocrr.2024.100745

Vincent D. de Jager MD , Léon C. van Kempen PhD , Betzabel N. Cajiao Garcia MSc , T. Jeroen N. Hiltermann MD, PhD , Anthonie J. van der Wekken MD, PhD , Ed Schuuring PhD , Stefan M. Willems MD, PhD

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Abstract

Introduction

Programmed death-ligand 1 (PD-L1) is the main predictive biomarker used to identify patients with NSCLC who are eligible for treatment with immune checkpoint inhibitors. Despite its utility, the predictive capacity of PD-L1 is limited, necessitating the exploration of supplementary predictive biomarkers. In this report, we describe the prognostic value of KRAS/TP53 mutation status for overall survival (OS) in patients with NSCLC treated with first-line immunotherapy or combined chemoimmunotherapy.

Methods

Clinical data of all patients diagnosed with metastatic nonsquamous NSCLC in the Netherlands between January 1 and December 31 of 2019 were retrieved from the Netherlands Cancer Registry and linked to pathology reports of the Dutch Nationwide Pathology Databank. A total of 694 patients with available KRAS and TP53 mutation status and treated with first-line pembrolizumab or chemoimmunotherapy were included, with a median follow-up time of 42.5 months. Patients with an EGFR or MET mutation or ALK, ROS1, or RET fusion were excluded from the analysis.

Results

Among patients treated with first-line pembrolizumab or chemoimmunotherapy, mutations in KRAS and TP53 occurred in 48.8% (n = 339) and 58.4% (n = 405), respectively. OS differed significantly between KRAS/TP53 mutational subgroups in patients treated with first-line pembrolizumab or chemoimmunotherapy (log-rank test, p = 0.007). Median OS of pembrolizumab or chemoimmunotherapy treated patients with mutated TP53 was longer in patients with KRAS-wildtype (485 versus 359 d, hazard ratio [HR] = 0.76, p = 0.028) or mutated KRAS (571 versus 447 d, HR = 0.73, p = 0.019). In a separate analysis of treatment subgroups, mutated TP53 was associated with longer median OS in chemoimmunotherapy treated KRAS-wildtype patients (468 versus 341 d, HR = 0.71, p = 0.029) but not in monoimmunotherapy treated patients with KRAS-wildtype (512 versus 371 d, HR = 0.91, p = 0.78). In multivariable Cox regression analysis including age, sex, clinical disease stage, and PD-L1 tumor proportion score, KRAS/TP53 mutation status was no longer associated with OS.

Conclusions

Among patients with metastatic NSCLC who are treated with pembrolizumab or chemoimmunotherapy, the presence of a pathogenic TP53 and KRAS mutation is associated with longer OS. Nevertheless, in multivariable Cox regression analysis including age, sex, clinical disease stage, and PD-L1 tumor proportion score, KRAS/TP53 mutation status was no longer associated with OS.

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在荷兰，KRAS/TP53 状态对一线单药免疫疗法和化疗免疫疗法治疗的非鳞状 NSCLC 患者总生存期的预后价值：简要报告

导言程序性死亡配体 1（PD-L1）是用于识别符合免疫检查点抑制剂治疗条件的 NSCLC 患者的主要预测性生物标志物。尽管PD-L1很有用，但其预测能力有限，因此有必要探索补充性预测生物标志物。在这份报告中，我们描述了KRAS/TP53突变状态对接受一线免疫疗法或联合化疗免疫疗法治疗的NSCLC患者总生存期（OS）的预后价值。方法从荷兰癌症登记处检索了2019年1月1日至12月31日期间在荷兰确诊的所有转移性非鳞状NSCLC患者的临床数据，并与荷兰全国病理数据库的病理报告相链接。共纳入了694名有KRAS和TP53突变状态、接受过pembrolizumab或化疗免疫疗法一线治疗的患者，中位随访时间为42.5个月。结果在接受一线pembrolizumab或化学免疫疗法治疗的患者中，KRAS和TP53突变发生率分别为48.8%（n = 339）和58.4%（n = 405）。在接受一线pembrolizumab或化学免疫疗法治疗的患者中，KRAS/TP53突变亚组之间的OS差异很大（对数秩检验，P = 0.007）。接受pembrolizumab或化学免疫疗法治疗的TP53突变患者的中位OS在KRAS-野生型（485天对359天，危险比[HR] = 0.76，p = 0.028）或KRAS突变（571天对447天，HR = 0.73，p = 0.019）患者中更长。在对治疗亚组的单独分析中，在接受化疗免疫治疗的KRAS-野生型患者中，突变的TP53与更长的中位OS相关（468对341 d，HR = 0.71，p = 0.029），但在接受单免疫治疗的KRAS-野生型患者中，突变的TP53与更长的中位OS无关（512对371 d，HR = 0.91，p = 0.78）。在包括年龄、性别、临床疾病分期和PD-L1肿瘤比例评分在内的多变量Cox回归分析中，KRAS/TP53突变状态与OS不再相关。结论在接受pembrolizumab或化学免疫疗法治疗的转移性NSCLC患者中，致病性TP53和KRAS突变的存在与较长的OS相关。然而，在包括年龄、性别、临床疾病分期和PD-L1肿瘤比例评分在内的多变量Cox回归分析中，KRAS/TP53突变状态与OS不再相关。

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

JTO Clinical and Research Reports Medicine-Oncology

CiteScore

4.20

自引率

0.00%

发文量

145

审稿时长

19 weeks