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Post surgery circulating free tumor DNA is a predictive biomarker for relapse of lung cancer

机译:手术后循环的游离肿瘤DNA是肺癌复发的预测生物标志物

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摘要

Cancer cells release DNA fragments into plasma as circulating free DNA (cfDNA). However, quantitative measurement of tumor‐derived DNA in cfDNA remains challenge. The purpose of this study was to quantitatively assess tumor‐derived DNA in lung cancer patients. By optimizing competitive allele‐specific TaqMan PCR (CAST‐PCR), we assessed the copy number of mutated Kirsten rat sarcoma viral oncogene homolog (KRAS) and epidermal growth factor receptor (EGFR) alleles in the pre/post surgery plasma of 168 lung cancer patients. An absolute quantitative PCR method was developed to assess the number of total cfDNA. All mutations detected in tumors were also found in the plasma after surgery. At the time of 30 days after surgery, EGFR mutation of circulating cell‐free DNA was detected only in two patients who recurred in 4 months after surgery. Compared to that of normal control at 30 days after surgery, five patients who recurred in 4 months had significantly higher circulating cell‐free DNA (P < 0.001), whereas six patients who recurred after 4 months (P = 0.207) and five patients without recurrence (P = 0.901) demonstrated significantly lower circulating cell‐free DNA. Our findings suggest that cfDNA analysis in plasma is an alternative and supplement to tissue analysis and hold promise for clinical application. Stratification of patients according to cfDNA levels at 30 days after surgery might be helpful in selecting lung cancer patients for adjuvant therapy after surgery.
机译:癌细胞将DNA片段以循环游离DNA(cfDNA)的形式释放到血浆中。然而,定量测量cfDNA中肿瘤来源的DNA仍然是一个挑战。这项研究的目的是定量评估肺癌患者的肿瘤来源的DNA。通过优化竞争性等位基因特异性TaqMan PCR(CAST-PCR),我们评估了168例肺癌术前/术后血浆中突变的Kirsten大鼠肉瘤病毒癌基因同源物(KRAS)和表皮生长因子受体(EGFR)等位基因的拷贝数耐心。开发了绝对定量PCR方法以评估总cfDNA的数量。手术后血浆中也发现了所有在肿瘤中检测到的突变。术后30天时,仅在术后4个月内复发的两名患者中检测到循环无细胞DNA的EGFR突变。与术后30天的正常对照相比,在4个月内复发的5例患者具有更高的循环无细胞DNA(P <0.001),而在4个月后复发的6例患者(P = 0.207)和5例无复发的患者复发(P = 0.901)显示循环的无细胞DNA明显降低。我们的发现表明血浆中的cfDNA分析是组织分析的替代和补充,并有望在临床上应用。在手术后30天根据cfDNA水平对患者进行分层可能有助于选择肺癌患者进行术后辅助治疗。

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