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首页> 外文期刊>Annals of the New York Academy of Sciences >Comparative Analysis of Mesenteric and Peripheral Blood Circulating Tumor DNA in Colorectal Cancer Patients
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Comparative Analysis of Mesenteric and Peripheral Blood Circulating Tumor DNA in Colorectal Cancer Patients

机译:大肠癌患者肠系膜和外周血循环肿瘤DNA的比较分析

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摘要

An increasing number of reports have demonstrated the presence of tumor-specific DNA in cancer patients' plasma/serum. These findings offer the prospective of serologic tumor markers that may aide in early disease detection, predict subclinical disease progression, and monitor treatment responses. However, for patients with colorectal cancer (CRC), there are few reports using this approach, with most revealing poor sensitivity. In contrast to tumors of other organ systems, CRCs drain predominantly via the mesenteric/portal veins (MV) to the liver. We hypothesize that because of this unique relation, tumor DNA may be less abundant in CRC patients' systemic circulation as compared to the mesenteric/portal system. At the time of surgery, paired blood was collected from both the peripheral vein (PV) and MV from 33 CRC patients. DNA was isolated from serum, quantified and assessed for loss of heterozygosity (LOH) using a panel of 11 microsatellite markers corresponding to regions on six chromosomes frequent for LOH in CRC. In addition, 16 samples were assessed for the presence of hypermethylated DNA for tumor suppressor genes: MGMT, P16, RAR-β2, RASSF1A, and APC. Circulating tumor DNA associated with LOH or methylation was more frequently detected in the MV of patients, 11 (33%) and 6 (38%), as compared to PV, 9 (27%) and 1 (6%), respectively. This study is the first to identify the presence of increased tumor DNA in the direct efferent venous drainage system of CRC and its variation as compared to systemic circulation. The findings provide important evidence supporting the origin of tumor-associated DNA in circulation, which merits consideration when devising blood-based nucleic acid assays for the assessment of CRC.
机译:越来越多的报告表明癌症患者血浆/血清中存在肿瘤特异性DNA。这些发现提供了血清学肿瘤标志物的前景,这些标志物可能有助于早期疾病检测,预测亚临床疾病进展并监测治疗反应。但是,对于结直肠癌(CRC)患者,很少有使用这种方法的报道,大多数都显示出较差的敏感性。与其他器官系统的肿瘤相反,CRC主要通过肠系膜/门静脉(MV)排入肝脏。我们假设由于这种独特的关系,与肠系膜/门静脉系统相比,CRC患者的全身循环中的肿瘤DNA可能较少。手术时,从33例CRC患者的外周静脉(PV)和MV中收集了配对的血液。从血清中分离DNA,定量并使用一组11个微卫星标记(对应于CRC中LOH频繁出现的六个染色体上的区域)评估杂合性(LOH)的损失。此外,评估了16个样品中抑癌基因MGMT,P16,RAR-β2,RASSF1A和APC的超甲基化DNA的存在。在患者的MV中,与LOH或甲基化相关的循环肿瘤DNA被检出的频率更高,分别为11(33%)和6(38%),而PV分别为9(27%)和1(6%)。这项研究是首次发现CRC的直接传出静脉引流系统中存在增加的肿瘤DNA及其与全身循环相比的变化。这些发现为循环中肿瘤相关DNA的起源提供了重要的证据,这在设计基于血液的核酸分析以评估CRC时值得考虑。

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