ctDNA-based minimal residual disease detection in lung cancer patients treated with curative intended chemoradiotherapy using a clinically transferable approach

Q3 Medicine

Cancer treatment and research communications Pub Date : 2024-01-01 DOI:10.1016/j.ctarc.2024.100802

Lærke Rosenlund Nielsen , Simone Stensgaard , Peter Meldgaard , Boe Sandahl Sorensen

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引用次数: 0

Abstract

Background

Reliable biomarkers are needed to identify tumor recurrence of non-small cell lung cancer (NSCLC) patients after chemoradiotherapy (CRT) with curative intent. This could improve consolidation therapy of progressing patients. However, the approach of existing studies has limited transferability to the clinic.

Materials and methods

A retrospective analysis of 135 plasma samples from 56 inoperable NSCLC patients who received CRT with curative intent was performed. Plasma samples collected at baseline, at the first check-up (average 1.6 months post-RT), and at the second check-up (average 4.5 months post-RT) were analyzed by deep sequencing with a commercially available cancer personalized profiling strategy (CAPP-Seq) using a tumor-agnostic approach.

Results

Detection of circulating tumor DNA (ctDNA) at 4.5 months after therapy was significantly associated with higher odds of tumor recurrence (OR: 5.4 (CI: 1.1–31), Fisher's exact test: p-value = 0.022), and shorter recurrence-free survival (RFS) (HR: 4.1 (CI: 1.7–10); log-rank test: p-value = 9e-04). In contrast, detection of ctDNA at 1.6 months after therapy was not associated with higher odds of tumor recurrence (OR: 2.7 (CI: 0.67–12), Fisher's exact test: p-value = 0.13) or shorter RFS (HR: 1.5 (CI: 0.67–3.3); log-rank test: p-value = 0.32).

Conclusion

This study demonstrates that the detection of ctDNA can be used to identify minimal residual disease 4.5 months after CRT in NSCLC patients using a commercially available kit and a tumor-agnostic approach. Furthermore, the time point of collecting the plasma sample after CRT has decisive importance for the prognostic value of ctDNA.

Micro abstract

This study analysed 135 plasma samples from 56 NSCLC patients treated with curative intent chemoradiotherapy using a tumor-agnostic approach. Detecting ctDNA at 4.5 months post-treatment was linked to higher recurrence odds, indicating ctDNA's potential as a biomarker for identifying residual disease after treatment with curative intent. Importantly, the study emphasizes the importance of timing for accurate ctDNA analysis results.

查看原文本刊更多论文

基于ctDNA的肺癌患者最小残留病检测，采用一种可临床移植的方法进行治疗性预期放化疗

背景需要可靠的生物标志物来识别非小细胞肺癌（NSCLC）患者在接受治愈性化疗（CRT）后的肿瘤复发情况。这可以改善进展期患者的巩固治疗。然而，现有研究的方法在临床上的可移植性有限。材料与方法对56名接受了以治愈为目的的CRT的不能手术的NSCLC患者的135份血浆样本进行了回顾性分析。对基线、首次检查（RT 后平均 1.6 个月）和第二次检查（RT 后平均 4.5 个月）收集的血浆样本进行了深度测序分析，采用的是市售的癌症个体化图谱分析策略（CAPP-Seq），采用的是肿瘤诊断方法。结果治疗后4.5个月检测到循环肿瘤DNA（ctDNA）与较高的肿瘤复发几率（OR：5.4（CI：1.1-31）；费雪精确检验：P值=0.022）和较短的无复发生存期（RFS）（HR：4.1（CI：1.7-10）；log-rank检验：P值=9e-04）显著相关。相反，治疗后 1.6 个月检测到 ctDNA 与肿瘤复发几率升高（OR：2.7 (CI：0.67-12)；费雪精确检验：P 值 = 0.13）或 RFS 缩短（HR：1.5 (CI：0.67-3.3)；对数秩检验：P 值 = 0.32）无关。结论本研究表明，使用市售试剂盒和肿瘤诊断方法，ctDNA检测可用于识别NSCLC患者CRT 4.5个月后的最小残留病。此外，CRT后收集血浆样本的时间点对ctDNA的预后价值具有决定性意义。微摘要这项研究采用肿瘤诊断方法分析了56名接受治愈性化疗的NSCLC患者的135份血浆样本。在治疗后4.5个月检测到ctDNA与较高的复发几率有关，这表明ctDNA有可能成为一种生物标志物，用于识别治愈性化疗后的残留疾病。重要的是，该研究强调了时机对准确的ctDNA分析结果的重要性。

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

Cancer treatment and research communications Medicine-Oncology

CiteScore

4.30

自引率

0.00%

发文量

148

审稿时长

56 days

期刊介绍： Cancer Treatment and Research Communications is an international peer-reviewed publication dedicated to providing comprehensive basic, translational, and clinical oncology research. The journal is devoted to articles on detection, diagnosis, prevention, policy, and treatment of cancer and provides a global forum for the nurturing and development of future generations of oncology scientists. Cancer Treatment and Research Communications publishes comprehensive reviews and original studies describing various aspects of basic through clinical research of all tumor types. The journal also accepts clinical studies in oncology, with an emphasis on prospective early phase clinical trials. Specific areas of interest include basic, translational, and clinical research and mechanistic approaches; cancer biology; molecular carcinogenesis; genetics and genomics; stem cell and developmental biology; immunology; molecular and cellular oncology; systems biology; drug sensitivity and resistance; gene and antisense therapy; pathology, markers, and prognostic indicators; chemoprevention strategies; multimodality therapy; cancer policy; and integration of various approaches. Our mission is to be the premier source of relevant information through promoting excellence in research and facilitating the timely translation of that science to health care and clinical practice.

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