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重复不稳定的新见解:RNA•DNA 杂交体的作用。

New insights into repeat instability: role of RNA•DNA hybrids.

机构信息

Department of Biochemistry and Molecular Biology and Center for Cancer Epigenetics, University of Texas MD Anderson Cancer Center, Houston, TX, USA.

出版信息

RNA Biol. 2010 Sep-Oct;7(5):551-8. doi: 10.4161/rna.7.5.12745. Epub 2010 Sep 1.

Abstract

Expansion of tandem repeat sequences is responsible for more than 20 human diseases. Several cis elements and trans factors involved in repeat instability (expansion and contraction) have been identified. However no comprehensive model explaining large intergenerational or somatic changes of the length of the repeating sequences exists. Several lines of evidence, accumulated from different model studies, indicate that transcription through repeat sequences is an important factor promoting their instability. The persistent interaction between transcription template DNA and nascent RNA (RNA•DNA hybrids, R loops) was shown to stimulate genomic instability. Recently, we demonstrated that cotranscriptional RNA•DNA hybrids are preferentially formed at GC-rich trinucleotide and tetranucleotide repeat sequences in vitro as well as in human genomic DNA. Additionally, we showed that cotranscriptional formation of RNA•DNA hybrids at CTG•CAG and GAA•TTC repeats stimulate instability of these sequences in both E. coli and human cells. Our results suggest that persistent RNA•DNA hybrids may also be responsible for other downstream effects of expanded trinucleotide repeats, including gene silencing. Considering the extent of transcription through the human genome as well as the abundance of GC-rich and/or non-canonical DNA structure forming tandem repeats, RNA•DNA hybrids may represent a common mutagenic conformation. Hence, R loops are potentially attractive therapeutic target in diseases associated with genomic instability.

摘要

串联重复序列的扩展是导致 20 多种人类疾病的原因。已经鉴定出涉及重复不稳定(扩展和收缩)的几个顺式元件和反式因子。然而,目前还没有一个全面的模型可以解释重复序列长度的大世代间或体细胞变化。从不同的模型研究中积累的几条证据表明,转录通过重复序列是促进其不稳定性的一个重要因素。研究表明,转录模板 DNA 与新生 RNA(RNA•DNA 杂交体,R 环)之间的持续相互作用会刺激基因组不稳定性。最近,我们证明了在体外和人基因组 DNA 中,富含 GC 的三核苷酸和四核苷酸重复序列优先形成共转录的 RNA•DNA 杂交体。此外,我们还表明,在 CTG•CAG 和 GAA•TTC 重复序列中形成共转录的 RNA•DNA 杂交体,会刺激这些序列在大肠杆菌和人类细胞中的不稳定性。我们的研究结果表明,持续的 RNA•DNA 杂交体也可能是扩展的三核苷酸重复序列的其他下游效应的原因之一,包括基因沉默。考虑到人类基因组中转录的程度,以及富含 GC 和/或形成串联重复的非典型 DNA 结构的丰度,RNA•DNA 杂交体可能代表一种常见的诱变构象。因此,R 环可能是与基因组不稳定性相关疾病的有吸引力的治疗靶点。

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