Andrea De Giglio , Dario De Biase , Valentina Favorito , Thais Maloberti , Alessandro Di Federico , Federico Zacchini , Giulia Venturi , Claudia Parisi , Filippo Gustavo Dall’Olio , Ilaria Ricciotti , Ambrogio Gagliano , Barbara Melotti , Francesca Sperandi , Annalisa Altimari , Elisa Gruppioni , Giovanni Tallini , Francesco Gelsomino , Lorenzo Montanaro , Andrea Ardizzoni
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Genomic aberrations such as <em>KRAS</em>, <em>TP53</em>, <em>KEAP1</em>, <em>SMARCA4</em>, or <em>STK11</em> may impact survival outcomes.</div></div><div><h3>Methods</h3><div>We performed an observational study of 145 patients treated with first-line IO or CT-ICI for advanced non-squamous (nsq) NSCLC at our institution tested with an extensive lab-developed NGS panel. The primary objective was to assess the clinical outcomes of STK11-mutated patients. Then, we performed an external validation through the public OAK/POPLAR dataset, including nsq NSCLC patients treated with single-agent ICI or CT.</div></div><div><h3>Results</h3><div>Most patients were male (59.7 %), former smokers (61.1 %), with ECOG PS 0–1 (84 %), and received first-line CT-IO (58.6 %). 44.8 % had a mutation in KRAS, 21.4 % in KEAP1, 50.3 % in TP53, 13.1 % in SMARCA4, and 14.4 % in the STK11 gene. The mOS was 8 mo. (95 % CI, 5–16.7) for STK11 mutated pts and 17.3 mo. for STK11 wild-type patients (95 % CI, 8.9–24.4) (p = 0.038). TP53 (8.3 vs 17.3), KRAS (9.2 vs 15.9), and KEAP1 (8.9 vs 15.9) mutated patients evidenced a trend for dismal mOS. SMARCA4 status had no impact on mOS. STK11 mutations were detrimental to OS in the univariate (HR 1.74, p = 0.041) and multivariate model (HR 1.97, p = 0.025) after adjusting for sex, age, ECOG PS, treatment (ICI vs CT-ICI), <em>KRAS</em>, <em>KEAP1</em>, <em>TP53</em>, and <em>SMARCA4</em> status. Genomic alterations did not impact the mPFS in our cohort. Within the OAK/POPLAR dataset, <em>STK11</em> mutations (60/818 pts) were significantly associated with increased death risk in the univariate (HR 2.01, p < 0.001) and multivariate model (HR 1.66, p = 0.001) after adjusting for age, sex, treatment (ICI vs CT), <em>KRAS</em>, <em>KEAP1</em>, <em>TP53</em>, and <em>SMARCA4</em> status.</div></div><div><h3>Conclusion</h3><div>STK11 aberrations hampered the mOS of nsq NSCLC patients treated with first-line ICI or CT-ICI. The negative prognostic impact seems to be unrelated to ICI administration.</div></div>","PeriodicalId":18129,"journal":{"name":"Lung Cancer","volume":"199 ","pages":"Article 108058"},"PeriodicalIF":4.5000,"publicationDate":"2025-01-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"STK11 mutations correlate with poor prognosis for advanced NSCLC treated with first-line immunotherapy or chemo-immunotherapy according to KRAS, TP53, KEAP1, and SMARCA4 status\",\"authors\":\"Andrea De Giglio , Dario De Biase , Valentina Favorito , Thais Maloberti , Alessandro Di Federico , Federico Zacchini , Giulia Venturi , Claudia Parisi , Filippo Gustavo Dall’Olio , Ilaria Ricciotti , Ambrogio Gagliano , Barbara Melotti , Francesca Sperandi , Annalisa Altimari , Elisa Gruppioni , Giovanni Tallini , Francesco Gelsomino , Lorenzo Montanaro , Andrea Ardizzoni\",\"doi\":\"10.1016/j.lungcan.2024.108058\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<div><h3>Background</h3><div>The upfront treatment of non-oncogene-addicted NSCLC relies on immunotherapy alone (ICI) or in combination with chemotherapy (CT-ICI). Genomic aberrations such as <em>KRAS</em>, <em>TP53</em>, <em>KEAP1</em>, <em>SMARCA4</em>, or <em>STK11</em> may impact survival outcomes.</div></div><div><h3>Methods</h3><div>We performed an observational study of 145 patients treated with first-line IO or CT-ICI for advanced non-squamous (nsq) NSCLC at our institution tested with an extensive lab-developed NGS panel. The primary objective was to assess the clinical outcomes of STK11-mutated patients. Then, we performed an external validation through the public OAK/POPLAR dataset, including nsq NSCLC patients treated with single-agent ICI or CT.</div></div><div><h3>Results</h3><div>Most patients were male (59.7 %), former smokers (61.1 %), with ECOG PS 0–1 (84 %), and received first-line CT-IO (58.6 %). 44.8 % had a mutation in KRAS, 21.4 % in KEAP1, 50.3 % in TP53, 13.1 % in SMARCA4, and 14.4 % in the STK11 gene. The mOS was 8 mo. (95 % CI, 5–16.7) for STK11 mutated pts and 17.3 mo. for STK11 wild-type patients (95 % CI, 8.9–24.4) (p = 0.038). TP53 (8.3 vs 17.3), KRAS (9.2 vs 15.9), and KEAP1 (8.9 vs 15.9) mutated patients evidenced a trend for dismal mOS. SMARCA4 status had no impact on mOS. STK11 mutations were detrimental to OS in the univariate (HR 1.74, p = 0.041) and multivariate model (HR 1.97, p = 0.025) after adjusting for sex, age, ECOG PS, treatment (ICI vs CT-ICI), <em>KRAS</em>, <em>KEAP1</em>, <em>TP53</em>, and <em>SMARCA4</em> status. Genomic alterations did not impact the mPFS in our cohort. 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引用次数: 0
摘要
背景:非癌基因成瘾NSCLC的前期治疗依赖于单独免疫治疗(ICI)或联合化疗(CT-ICI)。基因组畸变如KRAS、TP53、KEAP1、SMARCA4或STK11可能影响生存结果。方法:我们对我院145例接受一线IO或CT-ICI治疗晚期非鳞状(nsq) NSCLC的患者进行了一项观察性研究,并采用广泛的实验室开发的NGS面板进行了测试。主要目的是评估stk11突变患者的临床结果。然后,我们通过公共OAK/POPLAR数据集进行了外部验证,包括接受单药ICI或CT治疗的nsq NSCLC患者。结果:大多数患者为男性(59.7%),既往吸烟者(61.1%),ECOG PS 0-1(84%),接受一线CT-IO(58.6%)。KRAS基因突变占44.8%,KEAP1基因突变占21.4%,TP53基因突变占50.3%,SMARCA4基因突变占13.1%,STK11基因突变占14.4%。STK11突变患者的最大生存期为8个月(95% CI, 5-16.7), STK11野生型患者的最大生存期为17.3个月(95% CI, 8.9-24.4) (p = 0.038)。TP53 (8.3 vs 17.3)、KRAS (9.2 vs 15.9)和KEAP1 (8.9 vs 15.9)突变患者表现出令人沮丧的mOS趋势。SMARCA4状态对mOS无影响。在调整性别、年龄、ECOG PS、治疗(ICI vs CT-ICI)、KRAS、KEAP1、TP53和SMARCA4状态后,STK11突变在单变量模型(HR 1.74, p = 0.041)和多变量模型(HR 1.97, p = 0.025)中对OS有害。在我们的队列中,基因组改变没有影响mPFS。在OAK/POPLAR数据集中,STK11突变(60/818 pts)与单变量死亡风险增加显著相关(HR 2.01, p)。结论:STK11变异阻碍了一线ICI或CT-ICI治疗的nsq NSCLC患者的生存。负面预后影响似乎与ICI管理无关。
STK11 mutations correlate with poor prognosis for advanced NSCLC treated with first-line immunotherapy or chemo-immunotherapy according to KRAS, TP53, KEAP1, and SMARCA4 status
Background
The upfront treatment of non-oncogene-addicted NSCLC relies on immunotherapy alone (ICI) or in combination with chemotherapy (CT-ICI). Genomic aberrations such as KRAS, TP53, KEAP1, SMARCA4, or STK11 may impact survival outcomes.
Methods
We performed an observational study of 145 patients treated with first-line IO or CT-ICI for advanced non-squamous (nsq) NSCLC at our institution tested with an extensive lab-developed NGS panel. The primary objective was to assess the clinical outcomes of STK11-mutated patients. Then, we performed an external validation through the public OAK/POPLAR dataset, including nsq NSCLC patients treated with single-agent ICI or CT.
Results
Most patients were male (59.7 %), former smokers (61.1 %), with ECOG PS 0–1 (84 %), and received first-line CT-IO (58.6 %). 44.8 % had a mutation in KRAS, 21.4 % in KEAP1, 50.3 % in TP53, 13.1 % in SMARCA4, and 14.4 % in the STK11 gene. The mOS was 8 mo. (95 % CI, 5–16.7) for STK11 mutated pts and 17.3 mo. for STK11 wild-type patients (95 % CI, 8.9–24.4) (p = 0.038). TP53 (8.3 vs 17.3), KRAS (9.2 vs 15.9), and KEAP1 (8.9 vs 15.9) mutated patients evidenced a trend for dismal mOS. SMARCA4 status had no impact on mOS. STK11 mutations were detrimental to OS in the univariate (HR 1.74, p = 0.041) and multivariate model (HR 1.97, p = 0.025) after adjusting for sex, age, ECOG PS, treatment (ICI vs CT-ICI), KRAS, KEAP1, TP53, and SMARCA4 status. Genomic alterations did not impact the mPFS in our cohort. Within the OAK/POPLAR dataset, STK11 mutations (60/818 pts) were significantly associated with increased death risk in the univariate (HR 2.01, p < 0.001) and multivariate model (HR 1.66, p = 0.001) after adjusting for age, sex, treatment (ICI vs CT), KRAS, KEAP1, TP53, and SMARCA4 status.
Conclusion
STK11 aberrations hampered the mOS of nsq NSCLC patients treated with first-line ICI or CT-ICI. The negative prognostic impact seems to be unrelated to ICI administration.
期刊介绍:
Lung Cancer is an international publication covering the clinical, translational and basic science of malignancies of the lung and chest region.Original research articles, early reports, review articles, editorials and correspondence covering the prevention, epidemiology and etiology, basic biology, pathology, clinical assessment, surgery, chemotherapy, radiotherapy, combined treatment modalities, other treatment modalities and outcomes of lung cancer are welcome.
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