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首页> 外文期刊>Brazilian Journal of Pharmaceutical Sciences >Circulating cell-free DNA as a biomarker in the diagnosis and prognosis of colorectal cancer
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Circulating cell-free DNA as a biomarker in the diagnosis and prognosis of colorectal cancer

机译:循环中无细胞DNA作为大肠癌诊断和预后的生物标志物

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Colorectal cancer (CRC) is a disease without evident clinical symptoms in early stages, leading to late diagnosis and disease management. Current diagnostic and prognostic tools require invasive procedures and circulating molecular biomarkers fail to have optimal sensitivity and specificity. Circulating biomarkers with high clinical performance may be valuable for early diagnosis and prognosis of CRC. The purpose of this review was to investigate the application of circulating cell-free DNA (ccfDNA) in CRC diagnosis and prognosis and the analytical methods used in blood samples in articles published between 2005 and 2016. Based on specific inclusion and exclusion criteria, 26 articles were selected. Most studies used ccfDNA quantification as the molecular biomarker. The analytical method was mainly based on the quantitative polymerase chain reaction (qPCR). Biomarkers based on aberrantly methylated genes (n=6) and ccfDNA integrity/fragmentation (n=2) were also used for the CRC diagnosis. The CRC prognosis used the detection of oncogene mutations, such as KRAS and BRAF , in ccfDNA. Significant differences were found in variables among the studies revealing potential bias. ccfDNA quantification as a diagnostic biomarker for CRC has promising results but it lacks clinical specificity since other diseases present a similar increase in ccfDNA content. However, increasing research in the epigenomic field can lead the way to a clinically specific biomarker for the CRC early diagnosis. As for the analytical method, qPCR and derivatives seem to be a perfectly valid technique. The use of ccfDNA quantification in CRC prognosis seems promising. The attempt to use the ccfDNA quantification in clinical practice may reside in the prognosis using a qPCR technique.
机译:大肠癌(CRC)是一种在早期没有明显临床症状的疾病,导致晚期诊断和疾病管理。当前的诊断和预后工具需要侵入性程序,并且循环分子生物标志物不能具有最佳的敏感性和特异性。具有较高临床表现的循环生物标志物可能对CRC的早期诊断和预后有价值。这篇综述的目的是研究循环无细胞DNA(ccfDNA)在CRC诊断和预后中的应用以及在2005年至2016年间发表的文章中血液样本中使用的分析方法。基于具体的纳入和排除标准,共有26篇文章被选中。大多数研究使用ccfDNA定量作为分子生物标记。分析方法主要基于定量聚合酶链反应(qPCR)。基于异常甲基化基因(n = 6)和ccfDNA完整性/片段化(n = 2)的生物标记物也用于CRC诊断。 CRC预后用于检测ccfDNA中的癌基因突变,例如KRAS和BRAF。研究之间的变量之间存在显着差异,表明存在潜在偏见。 ccfDNA定量作为CRC的诊断生物标志物具有令人鼓舞的结果,但由于其他疾病的ccfDNA含量也有类似的增加,因此缺乏临床特异性。然而,在表基因组学领域的不断研究可以为CRC早期诊断提供一种临床上特定的生物标志物。至于分析方法,qPCR及其衍生物似乎是一种完全有效的技术。在CRC预后中使用ccfDNA定量似乎很有希望。在临床实践中使用ccfDNA定量分析的尝试可能存在于使用qPCR技术的预后中。

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