Department of Pathology and Laboratory Medicine, Weill Cornell Medicine, New York, New York, USA.
The Caryl and Israel Englander Institute for Precision Medicine, Weill Cornell Medicine and New York-Presbyterian, New York, New York, USA.
Oncologist. 2021 Nov;26(11):e1971-e1981. doi: 10.1002/onco.13905. Epub 2021 Aug 4.
Characterization of circulating tumor DNA (ctDNA) has been integrated into clinical practice. Although labs have standardized validation procedures to develop single locus tests, the efficacy of on-site plasma-based next-generation sequencing (NGS) assays still needs to be proved.
In this retrospective study, we profiled DNA from matched tissue and plasma samples from 75 patients with cancer. We applied an NGS test that detects clinically relevant alterations in 33 genes and microsatellite instability (MSI) to analyze plasma cell-free DNA (cfDNA).
The concordance between alterations detected in both tissue and plasma samples was higher in patients with metastatic disease. The NGS test detected 77% of sequence alterations, amplifications, and fusions that were found in metastatic samples compared with 45% of those alterations found in the primary tumor samples (p = .00005). There was 87% agreement on MSI status between the NGS test and tumor tissue results. In three patients, MSI-high ctDNA correlated with response to immunotherapy. In addition, the NGS test revealed an FGFR2 amplification that was not detected in tumor tissue from a patient with metastatic gastric cancer, emphasizing the importance of profiling plasma samples in patients with advanced cancer.
Our validation experience of a plasma-based NGS assay advances current knowledge about translating cfDNA testing into clinical practice and supports the application of plasma assays in the management of oncology patients with metastatic disease. With an in-house method that minimizes the need for invasive procedures, on-site cfDNA testing supplements tissue biopsy to guide precision therapy and is entitled to become a routine practice.
This study proposes a solution for decentralized liquid biopsy testing based on validation of a next-generation sequencing (NGS) test that detects four classes of genomic alterations in blood: sequence mutations (single nucleotide substitutions or insertions and deletions), fusions, amplifications, and microsatellite instability (MSI). Although there are reference labs that perform single-site comprehensive liquid biopsy testing, the targeted assay this study validated can be established locally in any lab with capacity to offer clinical molecular pathology assays. To the authors' knowledge, this is the first report that validates evaluating an on-site plasma-based NGS test that detects the MSI status along with common sequence alterations encountered in solid tumors.
循环肿瘤 DNA(ctDNA)的特征已被纳入临床实践。虽然实验室已经制定了标准化的验证程序来开发单基因座检测,但现场血浆的下一代测序(NGS)检测的有效性仍有待证明。
在这项回顾性研究中,我们对 75 名癌症患者的匹配组织和血浆样本进行了 DNA 分析。我们应用了一种 NGS 检测方法,该方法可检测 33 个基因和微卫星不稳定性(MSI)的临床相关改变,并分析血浆无细胞 DNA(cfDNA)。
在转移性疾病患者中,组织和血浆样本中检测到的改变具有更高的一致性。与原发性肿瘤样本相比,该 NGS 检测在转移性样本中检测到 77%的序列改变、扩增和融合,而在原发性肿瘤样本中仅检测到 45%(p =.00005)。该 NGS 检测与肿瘤组织结果在 MSI 状态上的一致性为 87%。在三名患者中,MSI 高 ctDNA 与免疫治疗反应相关。此外,该 NGS 检测还揭示了一名转移性胃癌患者的 FGFR2 扩增,而该患者的肿瘤组织中并未检测到,这强调了在晚期癌症患者中进行血浆样本分析的重要性。
我们对一种基于血浆的 NGS 检测方法的验证经验推进了将 cfDNA 检测转化为临床实践的相关知识,并支持在转移性疾病患者的肿瘤管理中应用血浆检测。通过一种内部方法,最大限度地减少了对侵入性程序的需求,现场 cfDNA 检测补充了组织活检以指导精准治疗,有资格成为常规实践。
本研究提出了一种基于下一代测序(NGS)检测的分散式液体活检检测的解决方案,该检测可检测血液中的四类基因组改变:序列突变(单核苷酸取代或插入和缺失)、融合、扩增和微卫星不稳定性(MSI)。虽然有参考实验室进行单站点综合液体活检检测,但本研究验证的靶向检测可在任何有能力提供临床分子病理检测的实验室中进行本地化建立。据作者所知,这是首次验证评估现场基于血浆的 NGS 检测的报告,该检测可检测 MSI 状态以及实体瘤中常见的序列改变。
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