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炎症反应中基因表达的表观遗传调控及其与常见疾病的相关性。

Epigenetic regulation of gene expression in the inflammatory response and relevance to common diseases.

作者信息

Wilson Anthony G

机构信息

Academic Rheumatology Group, School of Medicine and Biomedical Sciences, University of Sheffield, Beech Hill Road, Sheffield, U.K.

出版信息

J Periodontol. 2008 Aug;79(8 Suppl):1514-9. doi: 10.1902/jop.2008.080172.

Abstract

Epigenetics can be defined as all the meiotically and mitotically inherited changes in gene expression that are not encoded in the DNA sequence itself. Epigenetic modifications of chromatin and DNA have been recognized as important permissive and suppressive factors in controlling the expressed genome via gene transcription. Two major epigenetic mechanisms are the posttranslational modification of histone proteins in chromatin and the methylation of DNA itself, which are regulated by distinct, but coupled, pathways. It is clear that the epigenetic state is a central regulator of cellular development and activation. Emerging evidence suggests a key role for epigenetics in human pathologies, including in inflammatory and neoplastic disorders. The epigenome is influenced by environmental factors throughout life. Nutritional factors can have profound effects on the expression of specific genes by epigenetic modification, and these may be passed on to subsequent generations with potentially detrimental effects. Many cancers are associated with altered epigenetic profiles, leading to altered expression of the genes involved in cell growth or differentiation. Autoimmune and neoplastic diseases increase in frequency with increasing age, with epigenetic dysregulation proposed as a potential explanation. In support of this hypothesis, studies in monozygotic twins revealed increasing epigenetic differences with age. Differences in methylation status of CpG sites, monoallelic silencing, and other epigenetic regulatory mechanisms have been observed in key inflammatory response genes. The importance of the epigenome in the pathogenesis of common human diseases is likely to be as significant as that of traditional genetic mutations. With advances in technology, our understanding of this area of biology is likely to increase rapidly in the near future.

摘要

表观遗传学可定义为基因表达中所有经减数分裂和有丝分裂遗传的变化,这些变化并非由DNA序列本身编码。染色质和DNA的表观遗传修饰已被公认为是通过基因转录控制表达基因组的重要促进和抑制因素。两种主要的表观遗传机制是染色质中组蛋白的翻译后修饰和DNA本身的甲基化,它们由不同但相互关联的途径调控。很明显,表观遗传状态是细胞发育和激活的核心调节因子。新出现的证据表明表观遗传学在人类疾病中起关键作用,包括炎症性疾病和肿瘤性疾病。表观基因组在一生中都会受到环境因素的影响。营养因素可通过表观遗传修饰对特定基因的表达产生深远影响,并且这些影响可能会传递给后代,产生潜在的有害作用。许多癌症与表观遗传谱的改变有关,导致参与细胞生长或分化的基因表达改变。自身免疫性疾病和肿瘤性疾病的发病率随着年龄的增长而增加,表观遗传失调被认为是一种潜在的解释。支持这一假设的是,对同卵双胞胎的研究显示,随着年龄的增长,表观遗传差异不断增加。在关键的炎症反应基因中已观察到CpG位点甲基化状态、单等位基因沉默和其他表观遗传调控机制的差异。表观基因组在常见人类疾病发病机制中的重要性可能与传统基因突变的重要性相当。随着技术的进步,我们对这一生物学领域的理解在不久的将来可能会迅速增加。

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