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循环血浆游离DNA(cfDNA)作为放疗的预测生物标志物:一项头颈癌前瞻性试验的结果

Circulating Plasma Cell-free DNA (cfDNA) as a Predictive Biomarker for Radiotherapy: Results from a Prospective Trial in Head and Neck Cancer.

作者信息

Koukourakis Michael I, Xanthopoulou Erasmia, Koukourakis Ioannis M, Fortis Sotirios P, Kesesidis Nikolaos, Karakasiliotis Ioannis, Baxevanis Constantin N

机构信息

Department of Radiotherapy - Oncology, Medical School, Democritus University of Thrace, Alexandroupolis, Greece.

Radiation Oncology Unit, 1st Department of Radiology, Aretaieion University Hospital, Athens, Greece.

出版信息

Cancer Diagn Progn. 2023 Sep 3;3(5):551-557. doi: 10.21873/cdp.10254. eCollection 2023 Sep-Oct.

Abstract

BACKGROUND/AIM: The plasma levels of cell-free DNA (cfDNA) in cancer patients increase due to rapid cancer cell proliferation and death. Therefore, cfDNA can be used to study specific tumor-DNA features. In addition, the non-specific cfDNA concentration may be an important biomarker of cancer prognosis.

PATIENTS AND METHODS

We prospectively examined the predictive role of cfDNA levels and the kinetics in the outcome of chemo-radiotherapy (CRT) in a cohort of 47 patients with locally advanced squamous cell head-neck cancer (SCHNC) treated with definitive chemo-radiotherapy.

RESULTS

Increased cfDNA levels after therapy completion (after/before treatment ratio; A/B-ratio >1) were found in 26/47 patients (55.3%). Locally advanced T4-stage was significantly associated with higher cfDNA levels after CRT (3.3 ng/μl in T4-stage vs. 1.3 ng/μl in T1-3 stages, p=0.007). Patients who responded to CRT (partial/complete response) had significantly lower cfDNA levels before therapy (mean values 1.2 ng/μl vs. 2.7 ng/μl, p=0.03). A significantly worse locoregional progression-free survival in patients with an A/B-ratio >1 was documented (p=0.01; hazard ratio 3.5, 95%CI=1.2-9.7). This was also confirmed in multivariate analysis, where the A/B-ratio was an independent predictive variable of locoregional relapse (p=0.03, hazard ratio 3.9, 95%CI=1.2-13).

CONCLUSION

High post-CRT cfDNA levels could be an early biomarker for the immediate recruitment of patients with SCHNC in consolidation chemo-immunotherapy protocols.

摘要

背景/目的:由于癌细胞快速增殖和死亡,癌症患者血浆中游离DNA(cfDNA)水平会升高。因此,cfDNA可用于研究特定肿瘤DNA特征。此外,非特异性cfDNA浓度可能是癌症预后的重要生物标志物。

患者与方法

我们前瞻性地研究了47例接受根治性放化疗的局部晚期头颈部鳞状细胞癌(SCHNC)患者中,cfDNA水平及其动力学对放化疗(CRT)疗效的预测作用。

结果

47例患者中有26例(55.3%)在治疗完成后cfDNA水平升高(治疗后/治疗前比值;A/B比值>1)。局部晚期T4期与CRT后较高的cfDNA水平显著相关(T4期为3.3 ng/μl,T1-3期为1.3 ng/μl,p = 0.007)。对CRT有反应(部分/完全缓解)的患者在治疗前cfDNA水平显著较低(平均值分别为1.2 ng/μl和2.7 ng/μl,p = 0.03)。记录显示A/B比值>1的患者局部区域无进展生存期显著更差(p = 0.01;风险比3.5,95%置信区间=1.2 - 9.7)。多变量分析也证实了这一点,其中A/B比值是局部区域复发的独立预测变量(p = 0.03,风险比3.9,95%置信区间=1.2 - 13)。

结论

CRT后高cfDNA水平可能是将SCHNC患者立即纳入巩固性化疗免疫治疗方案的早期生物标志物。

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