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培养癌细胞释放的游离DNA的特征分析。

Characterization of the cell-free DNA released by cultured cancer cells.

作者信息

Bronkhorst Abel Jacobus, Wentzel Johannes F, Aucamp Janine, van Dyk Etresia, du Plessis Lissinda, Pretorius Piet J

机构信息

Centre for Human Metabolomics, Biochemistry Division, North-West University, Potchefstroom 2520, South Africa.

Centre of Excellence for Pharmaceutical Sciences (PHARMACEN), North-West University, Potchefstroom 2520, South Africa.

出版信息

Biochim Biophys Acta. 2016 Jan;1863(1):157-65. doi: 10.1016/j.bbamcr.2015.10.022. Epub 2015 Oct 31.

Abstract

The most prominent factor that delays the translation of cell-free DNA (cfDNA) analyses to clinical practice is the lack of knowledge regarding its origin and composition. The elucidation of the former is complicated by the seemingly random fluctuation of quantitative and qualitative characteristics of cfDNA in the blood of healthy and diseased individuals. Besides methodological discrepancies, this could be ascribed to a web of cellular responses to various environmental cues and stressors. Since all cells release cfDNA, it follows that the cfDNA in the blood of cancer patients is not only representative of tumor derived DNA, but also of DNA released by healthy cells under different conditions. Additionally, cfDNA released by malignant cells is not necessarily just aberrant, but likely includes non-mutated chromosomal DNA fragments. This may cause false positive/negative results. Although many have acknowledged that this is a major problem, few have addressed it. We propose that many of the current stumbling blocks encountered in in vivo cfDNA studies can be partially circumvented by in vitro models. Accordingly, the purpose of this work was to evaluate the release of cfDNA from cultured cells and to gauge its potential use for elucidating the nature of cfDNA. Results suggest that the occurrence of cfDNA is not a consequence of apoptosis or necrosis, but primarily a result of actively secreted DNA, perhaps in association with a protein complex. This study demonstrates the potential of in vitro cell culture models to obtain useful information about the phenomenon of cfDNA.

摘要

阻碍无细胞DNA(cfDNA)分析转化为临床实践的最突出因素是缺乏对其来源和组成的了解。健康个体和患病个体血液中cfDNA的定量和定性特征看似随机波动,这使得对其来源的阐释变得复杂。除了方法上的差异,这可能归因于细胞对各种环境信号和应激源的一系列反应。由于所有细胞都会释放cfDNA,因此癌症患者血液中的cfDNA不仅代表肿瘤来源的DNA,还代表不同条件下健康细胞释放的DNA。此外,恶性细胞释放的cfDNA不一定只是异常的,还可能包括未突变的染色体DNA片段。这可能导致假阳性/阴性结果。尽管许多人都承认这是一个主要问题,但很少有人解决它。我们认为,目前体内cfDNA研究中遇到的许多绊脚石可以通过体外模型部分规避。因此,这项工作的目的是评估培养细胞中cfDNA的释放,并评估其在阐明cfDNA性质方面的潜在用途。结果表明,cfDNA的出现不是凋亡或坏死的结果,而是主要是主动分泌DNA的结果,可能与一种蛋白质复合物有关。这项研究证明了体外细胞培养模型在获取有关cfDNA现象的有用信息方面的潜力。

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