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前突变亨廷顿等位基因采用非 B 构象,并包含 DNA 损伤热点。

Premutation huntingtin allele adopts a non-B conformation and contains a hot spot for DNA damage.

机构信息

Department of Chemistry, Brown University, Providence, RI 02912, USA.

出版信息

Biochem Biophys Res Commun. 2011 Dec 9;416(1-2):146-52. doi: 10.1016/j.bbrc.2011.11.013. Epub 2011 Nov 11.

Abstract

The expansion of a CAG trinucleotide repeat (TNR) sequence has been linked to several neurological disorders, for example, Huntington's disease (HD). In HD, healthy individuals have 5-35 CAG repeats. Those with 36-39 repeats have the premutation allele, which is known to be prone to expansion. In the disease state, greater than 40 repeats are present. Interestingly, the formation of non-B DNA conformations by the TNR sequence is proposed to contribute to the expansion. Here we provide the first structural and thermodynamic analysis of a premutation length TNR sequence. Using chemical probes of nucleobase accessibility, we found that similar to (CAG)(10), the premutation length sequence (CAG)(36) forms a stem-loop hairpin and contains a hot spot for DNA damage. Additionally, calorimetric analysis of a series of (CAG)(n) sequences, that includes repeat tracts in both the healthy and premutation ranges, reveal that thermodynamic stability increases linearly with the number of repeats. Based on these data, we propose that while non-B conformations can be formed by TNR tracts found in both the healthy and premutation allele, only sequences containing at least 36 repeats have sufficient thermodynamic stability to contribute to expansion.

摘要

CAG 三核苷酸重复序列(TNR)的扩展与几种神经退行性疾病有关,例如亨廷顿病(HD)。在 HD 中,健康个体的 CAG 重复数为 5-35。重复数为 36-39 的个体具有前突变等位基因,已知其容易扩展。在疾病状态下,存在大于 40 个重复。有趣的是,TNR 序列形成非 B 型 DNA 构象被认为有助于扩展。在这里,我们首次对前突变长度 TNR 序列进行了结构和热力学分析。使用核碱基可及性的化学探针,我们发现与(CAG)(10)相似,前突变长度序列(CAG)(36)形成茎环发夹结构,并包含 DNA 损伤热点。此外,对一系列(CAG)(n)序列的量热分析,包括健康和前突变范围内的重复片段,揭示了热力学稳定性随重复数呈线性增加。基于这些数据,我们提出,尽管在健康和前突变等位基因中都可以形成 TNR 片段的非 B 型构象,但只有包含至少 36 个重复的序列才具有足够的热力学稳定性来促进扩展。

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