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表观遗传学与三联体重复神经疾病

Epigenetics and Triplet-Repeat Neurological Diseases.

作者信息

Nageshwaran Sathiji, Festenstein Richard

机构信息

Division of Brain Sciences and MRC Clinical Sciences Centre, Faculty of Medicine, Imperial College London, Hammersmith Hospital Campus , London , UK.

出版信息

Front Neurol. 2015 Dec 21;6:262. doi: 10.3389/fneur.2015.00262. eCollection 2015.

Abstract

The term "junk DNA" has been reconsidered following the delineation of the functional significance of repetitive DNA regions. Typically associated with centromeres and telomeres, DNA repeats are found in nearly all organisms throughout their genomes. Repetitive regions are frequently heterochromatinized resulting in silencing of intrinsic and nearby genes. However, this is not a uniform rule, with several genes known to require such an environment to permit transcription. Repetitive regions frequently exist as dinucleotide, trinucleotide, and tetranucleotide repeats. The association between repetitive regions and disease was emphasized following the discovery of abnormal trinucleotide repeats underlying spinal and bulbar muscular atrophy (Kennedy's disease) and fragile X syndrome of mental retardation (FRAXA) in 1991. In this review, we provide a brief overview of epigenetic mechanisms and then focus on several diseases caused by DNA triplet-repeat expansions, which exhibit diverse epigenetic effects. It is clear that the emerging field of epigenetics is already generating novel potential therapeutic avenues for this group of largely incurable diseases.

摘要

随着对重复DNA区域功能重要性的明确,“垃圾DNA”这一术语已被重新审视。DNA重复序列通常与着丝粒和端粒相关,几乎在所有生物体的整个基因组中都能找到。重复区域常常发生异染色质化,导致内在基因和附近基因沉默。然而,这并非统一规律,已知有几个基因需要这样的环境来进行转录。重复区域通常以二核苷酸、三核苷酸和四核苷酸重复的形式存在。1991年发现脊髓和延髓性肌萎缩(肯尼迪病)以及脆性X智力低下综合征(FRAXA)背后存在异常三核苷酸重复后,重复区域与疾病之间的关联得到了强调。在本综述中,我们简要概述了表观遗传机制,然后重点关注由DNA三联体重复扩增引起的几种疾病,这些疾病表现出多样的表观遗传效应。显然,新兴的表观遗传学领域已经为这组基本上无法治愈的疾病开辟了新的潜在治疗途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cd8b/4685448/103ad1739b2d/fneur-06-00262-g001.jpg

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