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Technical advances in global DNA methylation analysis in human cancers

机译:人类癌症中全球DNA甲基化分析的技术进步

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摘要

Prototypical abnormalities of genome-wide DNA methylation constitute the most widely investigated epigenetic mechanism in human cancers. Errors in the cellular machinery to faithfully replicate the global 5-methylcytosine (5mC) patterns, commonly observed during tumorigenesis, give rise to misregulated biological pathways beneficial to the rapidly propagating tumor mass but deleterious to the healthy tissues of the affected individual. A growing body of evidence suggests that the global DNA methylation levels could serve as utilitarian biomarkers in certain cancer types. Important breakthroughs in the recent years have uncovered further oxidized derivatives of 5mC - 5-hydroxymethylcytosine (5hmC), 5-formylcytosine (5fC) and 5-carboxylcytosine (5caC), thereby expanding our understanding of the DNA methylation dynamics. While the biological roles of these epigenetic derivatives are being extensively characterized, this review presents a perspective on the opportunity of innovation in the global methylation analysis platforms. While multiple methods for global analysis of 5mC in clinical samples exist and have been reviewed elsewhere, two of the established methods - Liquid Chromatography coupled with mass spectrometry (LC-MS/MS) and Immunoquantification have successfully evolved to include the quantitation of 5hmC, 5fC and 5caC. Although the analytical performance of LC-MS/MS is superior, the simplicity afforded by the experimental procedure of immunoquantitation ensures it’s near ubiquity in clinical applications. Recent developments in spectroscopy, nanotechnology and sequencing also provide immense promise for future evaluations and are discussed briefly. Finally, we provide a perspective on the current scenario of global DNA methylation analysis tools and present suggestions to develop the next generation toolset.
机译:全基因组DNA甲基化的典型异常构成了人类癌症中研究最广泛的表观遗传机制。忠实复制总体5-甲基胞嘧啶(5mC)模式的细胞机制错误(通常在肿瘤发生期间观察到)会导致调节失调的生物途径,这有利于迅速繁殖的肿瘤块,但对受影响个体的健康组织有害。越来越多的证据表明,全球DNA甲基化水平可以用作某些癌症类型中的功利性生物标记。近年来的重要突破发现了5mC的进一步氧化衍生物-5-羟甲基胞嘧啶(5hmC),5-甲酰基胞嘧啶(5fC)和5-羧基胞嘧啶(5caC),从而扩展了我们对DNA甲基化动力学的理解。尽管对这些表观遗传衍生物的生物学作用进行了广泛表征,但本综述对全球甲基化分析平台中创新机会提出了看法。尽管存在多种用于临床样品中5mC全局分析的方法,并且已在其他地方进行了综述,但已建立的两种方法-液相色谱-质谱联用(LC-MS / MS)和免疫定量技术已成功发展为包括5hmC,5fC定量和5caC。尽管LC-MS / MS的分析性能优越,但免疫定量实验程序所提供的简便性确保了它在临床应用中几乎无处不在。光谱学,纳米技术和测序技术的最新发展也为未来的评估提供了广阔的前景,并进行了简要讨论。最后,我们提供了有关全球DNA甲基化分析工具当前情况的观点,并提出了开发下一代工具集的建议。

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