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成体干细胞中的 DNA 甲基化:自我更新的新见解。

DNA methylation in adult stem cells: new insights into self-renewal.

机构信息

Harvard Medical School.

Howard Hughes Medical Institute.

出版信息

Epigenetics. 2010 Apr;5(3):189-93. doi: 10.4161/epi.5.3.11374. Epub 2010 Apr 1.

Abstract

Methylation of cytosine residues in the context of CpG dinucleotides within mammalian DNA is an epigenetic modification with profound effects on transcriptional regulation. A group of enzymes, the DNA methyltransferases (DNMTs) tightly regulate both the initiation and maintenance of these methyl marks. Loss of critical components of this enzymatic machinery results in growth, viability, and differentiation defects in both mice and humans, supporting the notion that this epigenetic modification is essential for proper development. Beyond this, DNA methylation also provides a potent epigenetic mechanism for cellular memory needed to silence repetitive elements and preserve lineage specificity over repeated cell divisions throughout adulthood. Recent work highlighting the specialized roles of DNA methylation and methyltransferases in maintaining adult somatic stem cell function suggests that further dissection of these mechanisms will shed new light on the complex nature of self-renewal.

摘要

在哺乳动物 DNA 中的 CpG 二核苷酸背景下,胞嘧啶残基的甲基化是一种具有深远影响的转录调控的表观遗传修饰。一组酶,即 DNA 甲基转移酶(DNMTs),严格调控这些甲基标记的起始和维持。该酶机制的关键成分的缺失会导致小鼠和人类的生长、存活和分化缺陷,这支持了这种表观遗传修饰对正常发育至关重要的观点。除此之外,DNA 甲基化还为细胞记忆提供了一种有效的表观遗传机制,这种机制需要沉默重复元件,并在成年期的多次细胞分裂中保持谱系特异性。最近的工作强调了 DNA 甲基化和甲基转移酶在维持成年体干细胞功能方面的特殊作用,这表明对这些机制的进一步剖析将揭示自我更新的复杂本质。

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