Utility of tumor-informed circulating tumor DNA for detection of minimal residual disease after curative-intent therapy in localized pancreatic cancer

Erin M. Dickey , Mary P. Martos , Ujwal Yanala , Andres Corona , Nkiruka Ezenwajiaku , Joseph Pizzolato , Dido Franceschi , Alan S. Livingstone , Gretel Terrero , Caitlin A. Hester , Nipun B. Merchant , Jashodeep Datta , Peter J. Hosein
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Abstract

Introduction

Patients with localized PDAC have high recurrence rates even after curative-intent therapies. Detection of minimal residual disease (MRD) can inform prognosis and may be therapeutically actionable. Tumor-informed circulating tumor (ct)DNA has been shown to be useful for MRD detection in other cancers, but its utility in localized PDAC patients undergoing curative-intent therapy is not well established.

Methods

ctDNA samples (total 106) from 32 patients, following completion of all curative-intent therapy, were subjected to Signatera™ analysis (Natera, Inc.). Recurrence-free survival (RFS) data was calculated using Kaplan-Meier estimates. Data from three previously presented studies using the same platform were pooled for validation.

Results

In our cohort (n = 32), ctDNA positivity rate was 28.1 % (9/32) with a median follow-up time of 17.7 months (range 4–62). Median RFS was significantly lower in patients with positive ctDNA (3.6 vs. 29.0 months, p < 0.001; HR: 72.1 [8.6—604.9]). Correlation of positive ctDNA with radiographic recurrence showed a sensitivity of 47.4 % (9/19), specificity of 100 % (13/13), PPV of 100 % (9/9), and NPV of 56.5 % (13/23). In the pooled cohort (n = 172), sensitivity was 66.7 % (50/75), specificity 77.3 % (75/97), PPV 69.4 % (50/72), and NPV 75.0 % (75/100).

Conclusions

Positive tumor-informed ctDNA test shows a high specificity and PPV for radiographic recurrence and is associated with significantly worse RFS. However, sensitivity of the test remains low.

Synopsis

In patients with localized PDAC completing curative-intent therapies, tumor-informed ctDNA assessment shows high specificity for radiographic recurrence and is associated with worse RFS. However, sensitivity remains low and presents an opportunity for improved calibration of this platform.
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导言局部 PDAC 患者即使接受了治愈性治疗,复发率也很高。最小残留病(MRD)的检测可为预后提供信息,并可用于治疗。肿瘤信息循环肿瘤(ct)DNA已被证明可用于其他癌症的MRD检测,但其在接受根治性治疗的局部PDAC患者中的应用尚未得到充分证实。无复发生存期(RFS)数据采用 Kaplan-Meier 估计法计算。结果在我们的队列(n = 32)中,ctDNA阳性率为28.1%(9/32),中位随访时间为17.7个月(4-62个月)。ctDNA阳性患者的中位RFS明显较低(3.6个月 vs. 29.0个月,p < 0.001; HR: 72.1 [8.6-604.9])。ctDNA阳性与放射学复发的相关性显示,敏感性为47.4%(9/19),特异性为100%(13/13),PPV为100%(9/9),NPV为56.5%(13/23)。在汇总队列(n = 172)中,敏感性为 66.7 %(50/75),特异性为 77.3 %(75/97),PPV 为 69.4 %(50/72),NPV 为 75.0 %(75/100)。简介在完成治愈性治疗的局部 PDAC 患者中,肿瘤提示的 ctDNA 评估对放射学复发显示出较高的特异性,并与较差的 RFS 相关。然而,灵敏度仍然很低,这为改进该平台的校准提供了机会。
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