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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Circulating free DNA in plasma or serum as biomarker of carcinogenesis: Practical aspects and biological significance.
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Circulating free DNA in plasma or serum as biomarker of carcinogenesis: Practical aspects and biological significance.

机译:血浆或血清中游离DNA循环作为癌变的生物标志物:实践意义和生物学意义。

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摘要

The presence of small amounts of tumor DNA in cell free DNA (CFDNA) circulating in the plasma or serum of cancer patients was first demonstrated 30 years ago. Since then, overall plasma DNA concentration in cancer patients and genetic or epigenetic alterations specific to tumor DNA have been investigated in patients diagnosed with different types of cancer. The proportion of patients with altered CFDNA varies with the pathology and the nature of the marker. However, several studies have reported the presence of altered CFDNA in over 50% of cancer patients, suggesting that this marker may be common and amenable for a variety of clinical and epidemiological studies. Because the mechanisms and timing of CFDNA release in the blood stream are poorly understood, only few studies have addressed the use of CFDNA for early cancer detection or as a biomarker for mutagenesis and tumourigenesis in molecular epidemiology. In this review, we discuss the technical issues involved in obtaining, using and analyzing CFDNA in cancer or healthy subjects. We also summarize the literature available on the mechanisms of CDNA release as well as on cross-sectional or prospective studies aimed at assessing the clinical and biological significance of CFDNA. These studies show that, in some circumstances, CFDNA alterations are detectable ahead of cancer diagnosis, raising the possibility of exploiting them as biomarkers for monitoring cancer occurrence. Testing these hypotheses will require well-designed studies, assessing multiple markers with quantitative and sensitive methods, with adequate follow-up of subjects, and we provide recommendations for the development of such studies.
机译:30年前首次证明了在癌症患者血浆或血清中循环的无细胞DNA(CFDNA)中存在少量肿瘤DNA。自那时以来,已经在诊断出患有不同类型癌症的患者中研究了癌症患者的总体血浆DNA浓度以及特定于肿瘤DNA的遗传或表观遗传学改变。 CFDNA改变的患者比例随病理和标志物的性质而变化。但是,有几项研究报告了超过50%的癌症患者存在CFDNA改变,这表明该标志物可能是常见的,并且适用于各种临床和流行病学研究。由于对CFDNA在血流中释放的机制和时机了解甚少,因此,只有极少的研究涉及将CFDNA用于早期癌症检测或作为分子流行病学中诱变和肿瘤发生的生物标志物。在这篇综述中,我们讨论了在癌症或健康受试者中获取,使用和分析CFDNA涉及的技术问题。我们还总结了有关CDNA释放机制以及旨在评估CFDNA的临床和生物学意义的横断面或前瞻性研究的可用文献。这些研究表明,在某些情况下,可以在癌症诊断之前检测到CFDNA改变,从而增加了将其用作监测癌症发生的生物标记的可能性。要检验这些假设,就需要进行精心设计的研究,并通过定量和敏感的方法评估多个标记,并对受试者进行充分的随访,我们为开展此类研究提供建议。

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