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Proofreading and Secondary Structure Processing Determine the Orientation Dependence of CAG·CTG Trinucleotide Repeat Instability in Escherichia coli

机译:校对和二级结构处理确定了大肠杆菌中CAG·CTG三核苷酸重复不稳定性的方向依赖性

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摘要

Expanded CAG·CTG trinucleotide repeat tracts are associated with several human inherited diseases, including Huntington's disease, myotonic dystrophy, and spinocerebellar ataxias. Here we describe a new model system to investigate repeat instability in the Escherichia coli chromosome. Using this system, we reveal patterns of deletion instability consistent with secondary structure formation in vivo and address the molecular basis of orientation-dependent instability. We demonstrate that the orientation dependence of CAG·CTG trinucleotide repeat deletion is determined by the proofreading subunit of DNA polymerase III (DnaQ) in the presence of the hairpin nuclease SbcCD (Rad50/Mre11). Our results suggest that, although initiation of slippage can occur independently of CAG·CTG orientation, the folding of the intermediate affects its processing and this results in orientation dependence. We propose that proofreading is inefficient on the CTG-containing strand because of its ability to misfold and that SbcCD contributes to processing in a manner that is dependent on proofreading and repeat tract orientation. Furthermore, we demonstrate that transcription and recombination do not influence instability in this system.
机译:扩展的CAG·CTG三核苷酸重复序列与几种人类遗传性疾病有关,包括亨廷顿氏病,强直性营养不良和脊髓小脑性共济失调。在这里,我们描述了一种新的模型系统,以研究大肠杆菌染色体中的重复不稳定性。使用此系统,我们揭示了与体内二级结构形成一致的缺失不稳定性模式,并阐明了方向依赖性不稳定性的分子基础。我们证明,在发夹核酸酶SbcCD(Rad50 / Mre11)存在下,DNA聚合酶III(DnaQ)的校正亚基决定了CAG·CTG三核苷酸重复缺失的方向依赖性。我们的结果表明,尽管滑动的发生可以独立于CAG·CTG取向发生,但中间体的折叠会影响其加工过程,并导致取向依赖性。我们建议对包含CTG的链进行校对是无效的,因为它具有错误折叠的能力,并且SbcCD的处理方式取决于校对和重复方向。此外,我们证明转录和重组不会影响该系统中的不稳定性。

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