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DNA低甲基化与人类疾病

DNA hypomethylation and human diseases.

作者信息

Wilson Ann S, Power Barbara E, Molloy Peter L

机构信息

Preventative Health National Research Flagship, North Ryde, NSW, Australia.

出版信息

Biochim Biophys Acta. 2007 Jan;1775(1):138-62. doi: 10.1016/j.bbcan.2006.08.007. Epub 2006 Sep 1.

Abstract

Changes in human DNA methylation patterns are an important feature of cancer development and progression and a potential role in other conditions such as atherosclerosis and autoimmune diseases (e.g., multiple sclerosis and lupus) is being recognised. The cancer genome is frequently characterised by hypermethylation of specific genes concurrently with an overall decrease in the level of 5 methyl cytosine. This hypomethylation of the genome largely affects the intergenic and intronic regions of the DNA, particularly repeat sequences and transposable elements, and is believed to result in chromosomal instability and increased mutation events. This review examines our understanding of the patterns of cancer-associated hypomethylation, and how recent advances in understanding of chromatin biology may help elucidate the mechanisms underlying repeat sequence demethylation. It also considers how global demethylation of repeat sequences including transposable elements and the site-specific hypomethylation of certain genes might contribute to the deleterious effects that ultimately result in the initiation and progression of cancer and other diseases. The use of hypomethylation of interspersed repeat sequences and genes as potential biomarkers in the early detection of tumors and their prognostic use in monitoring disease progression are also examined.

摘要

人类DNA甲基化模式的变化是癌症发生和发展的一个重要特征,并且其在其他病症(如动脉粥样硬化和自身免疫性疾病,例如多发性硬化症和狼疮)中的潜在作用也正在被认识到。癌症基因组的特征通常是特定基因的高甲基化,同时5-甲基胞嘧啶水平总体下降。基因组的这种低甲基化在很大程度上影响DNA的基因间和内含子区域,特别是重复序列和转座元件,并且被认为会导致染色体不稳定和突变事件增加。本综述探讨了我们对癌症相关低甲基化模式的理解,以及染色质生物学理解方面的最新进展如何有助于阐明重复序列去甲基化的潜在机制。它还考虑了包括转座元件在内的重复序列的整体去甲基化以及某些基因的位点特异性低甲基化如何可能导致最终引发癌症和其他疾病的有害影响。还研究了将散布重复序列和基因的低甲基化用作肿瘤早期检测的潜在生物标志物及其在监测疾病进展中的预后用途。

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