循环肿瘤DNA(ctDNA)动态变化可预测转移性胃食管癌(mGEC)全身治疗2周后的早期治疗反应。
Circulating Tumor DNA (ctDNA) Dynamics Predict Early Response to Treatment in Metastasized Gastroesophageal Cancer (mGEC) After 2 Weeks of Systemic Treatment.
作者信息
Tatalovic Stefan, Doleschal Bernhard, Kupferthaler Alexander, Grundner Stephan, Burghofer Jonathan, Webersinke Gerald, Schwendinger Simon, Jukic Emina, Zschocke Johannes, Danhel Lorenz, Kirchweger Antonia, Havranek Lukas, Shalamberidze Demetre, Rezaie Daniel, Biebl Matthias, Rumpold Holger, Kirchweger Patrick
机构信息
Department of Surgery, Ordensklinikum Linz, 4010 Linz, Austria.
Medical Faculty, Johannes Kepler University Linz, 4020 Linz, Austria.
出版信息
Cancers (Basel). 2024 Nov 26;16(23):3960. doi: 10.3390/cancers16233960.
UNLABELLED
mGEC is associated with poor overall survival (OS) of approximately 4-10 months. CtDNA is emerging as a promising prognostic biomarker with high potential for early relapse detection. However, until now, there was little knowledge on serial ctDNA detection and its impact on early treatment evaluation and prognosis in mGEC.
METHODS
ctDNA detection (ddPCR) was carried out serially in 37 matched tissue (NGS) patients with mGEC prior to systemic treatment initiation and every two weeks thereafter until restaging (n = 173 samples). The results have been correlated with response to treatment (restaging CT), overall survival (OS), and progression-free survival (PFS).
RESULTS
The pretherapeutic detection rate was 77.8%. Response to treatment assessment was correct in 54.2% (pretherapeutically pos./neg.) and 85.7% (dynamics at week 4). Moreover, a decline in ctDNA (MAF in %) below 57.1% of the pretherapeutic value after 2 weeks of systemic treatment was accompanied by a sensitivity of 57.1% and a specificity of 90% (AUC = 0.73) for correct restaging assessment (response evaluation by CT after 3 months) evaluating 76.5% of patients correctly after only 2 weeks. In contrast to mere pretherapeutic ctDNA positivity ( = 0.445), a decline in ctDNA dynamics to under 57.1% of its initial value was significantly associated with OS (4.1 (95% Cl 2.1-6.1) vs. 13.6 (95% CI 10.4-16.6) months, < 0.001) and PFS (3.2 (1.9-4.5) vs. 9.5 (95% CI 5.5-13.5) months, = 0.001) after two weeks of treatment. Additionally, the change in detectability from positive pretherapeutic levels to negative during treatment was associated with similar survival as for patients who were always regarded as ctDNA-negative (9.5 (95%Cl 0.4-18.5) vs. 9.6 (95%Cl 1.3-17.9)). The absence of becoming undetectable was associated with worse survival (4.7 months).
CONCLUSIONS
ctDNA is a promising additional biomarker allowing for early evaluation of response to treatment and saving unevaluated treatment time for patients with mGEC, and could allow for an early change in treatment with anticipated prognostic benefit in the future.
未标记
黏液性上皮性卵巢癌(mGEC)与总体生存期(OS)较差相关,约为4 - 10个月。循环肿瘤DNA(ctDNA)正成为一种有前景的预后生物标志物,在早期复发检测方面具有很高潜力。然而,到目前为止,关于mGEC中ctDNA的连续检测及其对早期治疗评估和预后的影响知之甚少。
方法
对37例mGEC患者在开始全身治疗前及之后每两周进行一次ctDNA检测(数字滴度PCR),直至重新分期(共173个样本),同时对匹配组织进行二代测序(NGS)。结果与治疗反应(重新分期CT)、总生存期(OS)和无进展生存期(PFS)相关。
结果
治疗前检测率为77.8%。治疗反应评估在治疗前阳性/阴性组中正确率为54.2%,在第4周动态变化组中为85.7%。此外,全身治疗2周后ctDNA(突变等位基因频率,MAF)下降至低于治疗前值的57.1%,其对正确重新分期评估(3个月后通过CT进行反应评估)的敏感性为57.1%,特异性为90%(曲线下面积 = 0.73),仅2周后就能正确评估76.5%的患者。与单纯治疗前ctDNA阳性情况相比(P = 0.445),ctDNA动态下降至初始值的57.1%以下与OS(4.1(95%置信区间2.1 - 6.1)个月对13.6(95%置信区间10.4 - 16.6)个月,P < 0.001)和PFS(3.2(1.9 - 4.5)个月对9.5(95%置信区间5.5 - 13.5)个月,P = 0.001)显著相关。此外,治疗期间从治疗前阳性水平变为阴性的可检测性变化与始终被视为ctDNA阴性的患者具有相似的生存期(9.5(95%置信区间0.4 - 18.5)个月对9.6(95%置信区间1.3 - 17.9)个月)。未变为不可检测与较差的生存期(4.7个月)相关。
结论
ctDNA是一种有前景的附加生物标志物,可用于mGEC患者治疗反应的早期评估,节省未评估的治疗时间,并可能在未来实现早期治疗改变并带来预期的预后益处。
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