N.N. Petrov Institute of Oncology, St. Petersburg 197758, Russia.
City Cancer Center, St. Petersburg 197758, Russia.
Cancer Genet. 2021 Aug;256-257:165-178. doi: 10.1016/j.cancergen.2021.05.014. Epub 2021 May 28.
This study aimed to investigate factors, which influence the content of circulating tumor DNA (ctDNA).
398 serial plasma samples were collected within 1-7 consecutive days from patients with EGFR-mutated lung cancer (n = 13), RAS/RAF-mutated colorectal cancer (n = 54) and BRAF-mutated melanoma (n = 17), who presented with measurable tumor disease. The amount of ctDNA was determined by ddPCR.
Among 82 patients, who donated 2-6 serial plasma samples, 42 subjects were classified as ctDNA-positive; only 22% cases were mutation-positive across all consecutive tests, while 24/82 (29%) patients showed presence of mutated ctDNA in some but not all blood draws. Subjects with progressing tumors had higher probability of being detected ctDNA-positive as compared to patients, who responded to therapy or had stable disease (39/55 (71%) vs. 4/24 (17%); p = 0.0001). Our study failed to reveal the impact of the time of the day, recent meal or prior physical exercise on the results of ctDNA testing.
Presence of ctDNA in plasma is particularly characteristic for patients, who experience clinical progression of tumor disease. Consecutive plasma tests may occasionally provide discordant data; thus, the repetition of analysis may be advised in certain cases in order to ensure the validity of negative ctDNA result.
本研究旨在探讨影响循环肿瘤 DNA(ctDNA)含量的因素。
从患有 EGFR 突变型肺癌(n=13)、RAS/RAF 突变型结直肠癌(n=54)和 BRAF 突变型黑色素瘤(n=17)的可测量肿瘤疾病患者中,在 1-7 天内连续采集 398 份血浆样本。采用 ddPCR 法测定 ctDNA 含量。
在 82 名捐赠 2-6 份连续血浆样本的患者中,42 例被分类为 ctDNA 阳性;仅在所有连续检测中,22%的病例为突变阳性,而 82 例患者中的 24/82(29%)在部分而非所有血液样本中存在突变 ctDNA。与对治疗有反应或疾病稳定的患者相比,肿瘤进展患者检测到 ctDNA 阳性的可能性更高(39/55(71%)比 4/24(17%);p=0.0001)。我们的研究未能揭示一天中的时间、最近的用餐或之前的体育锻炼对 ctDNA 检测结果的影响。
ctDNA 在血浆中的存在特别与肿瘤疾病临床进展的患者有关。连续的血浆检测偶尔可能会提供不一致的数据;因此,建议在某些情况下重复分析,以确保阴性 ctDNA 结果的有效性。
