在接受化疗、免疫疗法或靶向药物治疗的肺癌中,组织非特异性循环肿瘤DNA反应监测的真实世界有效性
Real-World Validity of Tissue-Agnostic Circulating Tumor DNA Response Monitoring in Lung Cancers Treated With Chemotherapy, Immunotherapy, or Targeted Agents.
作者信息
Chiang Anne C, Madison Russell W, Assaf Zoe June, Fine Alexander, Cao Yi, Gjoerup Ole, Huang Yanmei, Jin Dexter X, Hughes Jason, Antic Vladan, Young Amanda, Fabrizio David, Shames David, Maund Sophia, Exarchos Alexia, Lakhanpal Shailendra, Zuniga Richard, Pasquina Lincoln W, Schulze Katja
机构信息
Yale School of Medicine, Department of Medicine, Section of Medical Oncology, New Haven, Connecticut.
Foundation Medicine, Inc., Cambridge, Massachusetts.
出版信息
JTO Clin Res Rep. 2025 Mar 19;6(9):100829. doi: 10.1016/j.jtocrr.2025.100829. eCollection 2025 Sep.
INTRODUCTION
Circulating tumor DNA (ctDNA) monitoring is emerging as a minimally invasive complement to tumor imaging. We evaluated the validity of tissue-agnostic ctDNA quantification across four treatment modalities in NSCLC and SCLC.
METHODS
Data from consenting patients were collected from electronic health records as part of the Prospective Clinico-Genomic study (NCT04180176). ctDNA tumor fraction (TF) was retrospectively calculated for plasma collected six to 15 weeks after therapy initiation. TF dynamics were compared among an exploratory cohort, NSCLC and SCLC validity cohorts, and by therapy class.
RESULTS
In on-treatment plasma, undetectable TF was associated with longer real-world progression-free survival and real-world overall survival in exploratory (21.8 versus 8.8 mo; hazard ratio [HR] = 0.35, 95% confidence interval [CI]: 0.24-0.50), validity NSCLC (23.5 versus 9.5 mo; HR = 0.34, 95% CI: 0.22-0.53), and validity SCLC (15.9 versus 8.3 mo; HR = 0.19, 95% CI: 0.08-0.42) cohorts. Equal to or greater than 90% and equal to or greater than 50% TF reduction from baseline was also associated with significantly improved outcomes. ctDNA dynamics differed by treatment class: TF reported greater discriminatory power for selecting tumor responses to immunotherapy and targeted therapy (≥50% decrease in 91% of responders versus 24% of nonresponders) than chemotherapy and chemo-immunotherapy (86% versus 60%). TF dynamics correlated with outcomes, but models of real-world progression-free survival and real-world overall survival were improved when tumor response was included.
CONCLUSIONS
Tissue-agnostic monitoring of molecular response on the basis of ctDNA TF dynamics has utility in the real-world setting across four different treatment regimens. These results suggest that ctDNA dynamics may be complementary to tumor imaging in both NSCLC and SCLC to better inform patient care.
引言
循环肿瘤DNA(ctDNA)监测正成为肿瘤成像的一种微创补充手段。我们评估了在非小细胞肺癌(NSCLC)和小细胞肺癌(SCLC)中,跨四种治疗方式进行组织非依赖性ctDNA定量分析的有效性。
方法
作为前瞻性临床基因组研究(NCT04180176)的一部分,从电子健康记录中收集了同意参与研究的患者的数据。回顾性计算治疗开始后6至15周采集的血浆中的ctDNA肿瘤分数(TF)。在一个探索性队列、NSCLC和SCLC有效性队列中,并按治疗类别比较TF动态变化。
结果
在治疗期间的血浆中,检测不到TF与探索性队列(21.8个月对8.8个月;风险比[HR]=0.35,95%置信区间[CI]:0.24-0.50)、有效性NSCLC队列(23.5个月对9.5个月;HR=0.34,95%CI:0.22-0.53)和有效性SCLC队列(15.9个月对8.3个月;HR=0.19,95%CI:0.08-0.42)中更长的实际无进展生存期和实际总生存期相关。从基线降低等于或大于90%以及等于或大于50%的TF也与显著改善的预后相关。ctDNA动态变化因治疗类别而异:与化疗和化疗免疫疗法(86%对60%)相比,TF在选择对免疫疗法和靶向疗法的肿瘤反应方面(91%的反应者与24%的无反应者相比有≥50%的降低)显示出更大的鉴别能力。TF动态变化与预后相关,但当纳入肿瘤反应时,实际无进展生存期和实际总生存期的模型得到了改善。
结论
基于ctDNA TF动态变化的组织非依赖性分子反应监测在四种不同治疗方案的实际应用中具有实用价值。这些结果表明ctDNA动态变化在NSCLC和SCLC中可能是肿瘤成像的补充手段,以更好地指导患者护理。
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