Concordance of circulating tumor DNA and matched formalin-fixed paraffin-embedded tumor tissue in gastric cancer as a predictor of recurrence.

Korean journal of clinical oncology Pub Date : 2023-12-01 Epub Date: 2023-12-31 DOI:10.14216/kjco.23009
Soo Hyun Seo, Young Suk Park, Soo Kyung Nam, Hye Seung Lee, Do Joong Park, Kyoung Un Park
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Abstract

Purpose: Combined analysis of the variant composition of circulating tumor DNA (ctDNA) from cell-free plasma and DNA from tumor tissue could provide insight into the implications of the genetic alterations responsible for the intratumoral and intertumoral heterogeneity of gastric cancer. We aimed to evaluate the usefulness of this approach in these patients.

Methods: Cell-free plasma and formalin-fixed paraffin-embedded tumor tissue samples from 46 patients with gastric cancer were examined. Targeted deep sequencing was performed using a commercially available kit.

Results: The cell-free DNA (cfDNA) concentration was higher in stage II-IV versus stage I patients and in larger versus smaller tumors. Only 12 of the 36 (33.3%) alterations in the tumor tissue samples were in concordance with those in the ctDNA samples. Two variants were in concordance in stage I samples and 10 in stage II-IV samples. Actionable variants that were detected in concordance were in the stage II-IV samples. Preoperative ctDNA positivity of actionable variants was significantly associated with cfDNA concentration, lymphatic invasion, N stage, and TNM stage. Cancer recurrence was significantly associated with tumor size, lymphatic/vascular invasion, TNM stage, and ctDNA-tumor tissue variant concordance.

Conclusion: Preoperative ctDNA genetic analysis using a multigene panel offers substantial clinical benefits when performed in conjunction with targeted deep sequencing of tumor tissue. Concordance between preoperative ctDNA and tumor tissue mutations may serve as a prognostic indicator in patients with gastric cancer.

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胃癌循环肿瘤 DNA 与匹配的福尔马林固定石蜡包埋肿瘤组织的一致性作为复发的预测指标
目的:对来自无细胞血浆的循环肿瘤 DNA (ctDNA) 和来自肿瘤组织的 DNA 的变异成分进行联合分析,可以深入了解导致胃癌瘤内和瘤间异质性的基因改变的影响。我们的目的是评估这种方法在这些患者中的实用性:方法:我们研究了 46 位胃癌患者的无细胞血浆和福尔马林固定石蜡包埋肿瘤组织样本。使用市售试剂盒进行了靶向深度测序:结果:II-IV期患者的无细胞DNA(cfDNA)浓度高于I期患者,肿瘤较大的患者的无细胞DNA浓度高于肿瘤较小的患者。肿瘤组织样本中的 36 个变异中只有 12 个(33.3%)与 ctDNA 样本中的变异一致。I 期样本中有两个变异是一致的,II-IV 期样本中有 10 个。II-IV期样本中检测到的可操作变异是一致的。术前ctDNA阳性可操作变异与cfDNA浓度、淋巴侵袭、N分期和TNM分期显著相关。癌症复发与肿瘤大小、淋巴/血管侵犯、TNM分期以及ctDNA-肿瘤组织变异一致性有明显相关性:结论:使用多基因面板进行术前ctDNA基因分析,并结合肿瘤组织靶向深度测序,可为临床带来巨大益处。术前ctDNA与肿瘤组织变异的一致性可作为胃癌患者的预后指标。
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