Inter-Department Program of Biomedical Sciences, Faculty of Graduate School, Chulalongkorn University, Bangkok, Thailand.
J Cancer Res Clin Oncol. 2013 Jan;139(1):67-76. doi: 10.1007/s00432-012-1300-5. Epub 2012 Aug 25.
A high level of circulating DNA (cirDNA) in cancer patients has been correlated with poor outcomes. Studies have demonstrated the critical contributions of the tumor-derived cirDNA. In this report, we investigated the roles of the non-tumor-derived cirDNA (nt-cirDNA) in determining the prognosis of non-small cell lung cancer (NSCLC).
Plasma samples from 58 advanced NSCLC patients and 52 controls were collected. The nt-cirDNA levels were assessed with qPCR assay to detect the unmethylation status of an epithelial-specific marker, the SHP-1 promoter 2 (unmethylated SHP1P2). Clinicopathological correlations were analyzed.
There was a significant increase in the total amount of cirDNA in NSCLC patients compared with controls: 4.3 ng ml(-1) [0.82-49.8] and 2.0 ng ml(-1) [0.03-26.9], respectively (p < 0.01). An increased amount of the unmethylated SHP1P2 in advanced NSCLC was also detected: 3.4 ng ml(-1) [1.2-24.8] versus 2.0 ng ml(-1) [0.03-26.9] in the controls (p = 0.026). Survival analyses revealed that high levels of total cirDNA and unmethylated SHP1P2 were significantly associated with decreased survival. However, the total cirDNA had a better prognostic correlation than the unmethylated SHP1P2. Multivariate analysis identified total cirDNA (p = 0.004) and systemic treatment (p = 0.002) as independent prognostic parameters.
The level of total cirDNA in NSCLC is an important prognostic parameter that demonstrates the contributions from both tumor-derived sources and non-tumor-derived sources.
癌症患者的循环 DNA(cirDNA)水平较高与不良预后相关。研究表明肿瘤源性 cirDNA 具有重要作用。在本报告中,我们研究了非肿瘤源性 cirDNA(nt-cirDNA)在确定非小细胞肺癌(NSCLC)患者预后中的作用。
收集了 58 例晚期 NSCLC 患者和 52 例对照者的血浆样本。采用 qPCR 法检测上皮细胞特异性标志物 SHP-1 启动子 2(未甲基化 SHP1P2)的 unmethylation 状态,评估 nt-cirDNA 水平。分析临床病理相关性。
与对照组相比,NSCLC 患者的总 cirDNA 量显著增加:分别为 4.3ng/ml(0.82-49.8)和 2.0ng/ml(0.03-26.9)(p<0.01)。还检测到晚期 NSCLC 中未甲基化 SHP1P2 的量增加:分别为 3.4ng/ml(1.2-24.8)和 2.0ng/ml(0.03-26.9)(p=0.026)。生存分析显示,总 cirDNA 和未甲基化 SHP1P2 水平高与生存时间缩短显著相关。然而,总 cirDNA 与预后的相关性优于未甲基化 SHP1P2。多变量分析确定总 cirDNA(p=0.004)和全身治疗(p=0.002)为独立的预后参数。
NSCLC 中总 cirDNA 水平是一个重要的预后参数,表明其来源于肿瘤源性和非肿瘤源性来源。
