循环甲基化标记物对直肠癌抗肿瘤治疗的动态变化

IF 1.6 Q4 ONCOLOGY

Journal of Gastrointestinal Cancer Pub Date : 2024-09-01 Epub Date: 2024-06-03 DOI:10.1007/s12029-024-01066-y

Anastasia A Ponomaryova, Elena Yu Rykova, Anastasia I Solovyova, Anna S Tarasova, Dmitry N Kostromitsky, Alexey Yu Dobrodeev, Sergey A Afanasiev, Nadezhda V Cherdyntseva

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Aberrant methylation of tumor-suppressor genes and hypomethylation of retrotransposons were shown to be detectable in cell-free DNA, circulating in the blood (cfDNA) of cancer patients, indicating the possibility to use them as diagnostic and prognosis markers.Purpose: Evaluation of the changes in the methylation level of LINE-1 elements and SEPTIN9 and IKZF1 genes in the cell-surface-bound cfDNA (csb-cfDNA) from the blood of RC patients after antitumor therapy at a long-term follow-up.Methods: Blood samples were obtained from RC patients (n = 25) before treatment, after preoperative chemotherapy (3 courses according to the XELOX scheme), 10-15 days after surgery, and every 3 months during 12 months of dynamic observation. 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引用次数: 0

摘要

背景：直肠癌（RC）在肿瘤发病率和死亡率结构中占据主导地位。在癌症患者血液中循环的无细胞 DNA（cfDNA）中可检测到肿瘤抑制基因的异常甲基化和逆转录转座子的低甲基化，这表明有可能将它们用作诊断和预后标志物。目的：在长期随访中评估抗肿瘤治疗后 RC 患者血液中细胞表面结合的 cfDNA（csb-cfDNA）中 LINE-1 元件、SEPTIN9 和 IKZF1 基因甲基化水平的变化：方法：在治疗前、术前化疗（根据 XELOX 方案进行 3 个疗程）后、术后 10-15 天以及 12 个月的动态观察期间，每隔 3 个月从 RC 患者（n = 25）处采集血液样本。通过甲基特异性定量 PCR 评估 csb-cfDNA 中 LINE-1、SEPTIN9 和 IKZF1 的甲基化水平：结果：与治疗前相比，RC 患者化疗后 csb-cfDNA 中 LINE-1 甲基化水平增加了 1.6 倍，肿瘤切除后增加了 3 倍。与治疗前相比，RC 患者化疗后 csb-cfDNA 中 SEPTIN9 基因甲基化水平下降了 1.7 倍，肿瘤切除后下降了 2.3 倍。联合治疗后，RC 患者的 IKZF1 基因甲基化水平下降了 2 倍。值得注意的是，与术后 10-15 天的水平相比，所有复发患者（n = 5）的 SEPTIN9 和 IKZF1 基因甲基化水平都有所提高，LINE-1 基因甲基化水平降低了 2 倍或更多。在对未复发的RC患者（n = 20）进行联合治疗后的12个月随访期间，循环中的SEPTIN9、IKZF1和LINE-1甲基化水平没有变化：结果表明，csb-cfDNA中的SEPTIN9、IKZF1和LINE-1甲基化水平是RC患者抗肿瘤治疗效果和早期发现复发的潜在标志物。

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Dynamic Changes in Circulating Methylated Markers in Response to Antitumor Therapy of Rectal Cancer.

Background: Rectal cancer (RC) occupies a leading position in the structure of oncological morbidity and mortality. Aberrant methylation of tumor-suppressor genes and hypomethylation of retrotransposons were shown to be detectable in cell-free DNA, circulating in the blood (cfDNA) of cancer patients, indicating the possibility to use them as diagnostic and prognosis markers.

Purpose: Evaluation of the changes in the methylation level of LINE-1 elements and SEPTIN9 and IKZF1 genes in the cell-surface-bound cfDNA (csb-cfDNA) from the blood of RC patients after antitumor therapy at a long-term follow-up.

Methods: Blood samples were obtained from RC patients (n = 25) before treatment, after preoperative chemotherapy (3 courses according to the XELOX scheme), 10-15 days after surgery, and every 3 months during 12 months of dynamic observation. The methylation level of LINE-1, SEPTIN9, and IKZF1 in the csb-cfDNA was evaluated by quantitative methyl-specific PCR.

Results: The LINE-1 methylation level in the csb-cfDNA increased 1.6 times in RC patients after chemotherapy and 3 times after tumor resection versus methylation level before therapy. The SEPTIN9 gene methylation level in the csb-cfDNA decreased by 1.7 times in RC patients after chemotherapy and by 2.3 times after tumor resection compared with the values before the treatment. The IKZF1 gene methylation level decreased by 2 times in RC patients after combined therapy. Notably, all patients with relapses (n = 5) showed an increase in methylation level for the SEPTIN9 and IKZF1 genes and a decrease of methylation level for the LINE-1 elements by 2 times or more in comparison with the level 10-15 days after surgery. There were no changes in the circulating SEPTIN9, IKZF1, and LINE-1 methylation levels during the 12-month follow-up period after the combined therapy of RC patients (n = 20) without relapses.

Conclusion: The results indicate that SEPTIN9, IKZF1, and LINE-1 methylation levels in the csb-cfDNA are potential markers of the effectiveness of antitumor therapy and early detection of relapse in RC patients.

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来源期刊

Journal of Gastrointestinal Cancer ONCOLOGY-

CiteScore

3.80

自引率

0.00%

发文量

121

期刊介绍： The Journal of Gastrointestinal Cancer is a multidisciplinary medium for the publication of novel research pertaining to cancers arising from the gastrointestinal tract.The journal is dedicated to the most rapid publication possible.The journal publishes papers in all relevant fields, emphasizing those studies that are helpful in understanding and treating cancers affecting the esophagus, stomach, liver, gallbladder and biliary tree, pancreas, small bowel, large bowel, rectum, and anus. In addition, the Journal of Gastrointestinal Cancer publishes basic and translational scientific information from studies providing insight into the etiology and progression of cancers affecting these organs. New insights are provided from diverse areas of research such as studies exploring pre-neoplastic states, risk factors, epidemiology, genetics, preclinical therapeutics, surgery, radiation therapy, novel medical therapeutics, clinical trials, and outcome studies.In addition to reports of original clinical and experimental studies, the journal also publishes: case reports, state-of-the-art reviews on topics of immediate interest or importance; invited articles analyzing particular areas of pancreatic research and knowledge; perspectives in which critical evaluation and conflicting opinions about current topics may be expressed; meeting highlights that summarize important points presented at recent meetings; abstracts of symposia and conferences; book reviews; hypotheses; Letters to the Editors; and other items of special interest, including:Complex Cases in GI Oncology: This is a new initiative to provide a forum to review and discuss the history and management of complex and involved gastrointestinal oncology cases. The format will be similar to a teaching case conference where a case vignette is presented and is followed by a series of questions and discussion points. A brief reference list supporting the points made in discussion would be expected.