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Hairpins are formed by the single DNA strands of the fragile X triplet repeats: structure and biological implications.

机译:发夹由脆弱的X三联体重复序列的单条DNA链形成:结构和生物学意义。

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摘要

Inordinate expansion and hypermethylation of the fragile X DNA triplet repeat, (GGC)n.(GCC)n, are correlated with the ability of the individual G- and C-rich single strands to form hairpin structures. Two-dimensional NMR and gel electrophoresis studies show that both the G- and C-rich single strands form hairpins under physiological conditions. This propensity of hairpin formation is more pronounced for the C-rich strand than for the G-rich strand. This observation suggests that the C-rich strand is more likely to form hairpin or "slippage" structure and show asymmetric strand expansion during replication. NMR data also show that the hairpins formed by the C-rich strands fold in such a way that the cytosine at the CpG step of the stem is C.C paired. The presence of a C.C mismatch at the CpG site generates local flexibility, thereby providing analogs of the transition to the methyltransferase. In other words, the hairpins of the C-rich strand act as better substrates for the human methyltransferase than the Watson-Crick duplex or the G-rich strand. Therefore, hairpin formation could account for the specific methylation of the CpG island in the fragile X repeat that occurs during inactivation of the FMR1 gene during the onset of the disease.
机译:脆弱的X DNA三联体重复序列(GGC)n。(GCC)n的过度扩增和甲基化过度与单个富含G和C的单链形成发夹结构的能力有关。二维NMR和凝胶电泳研究表明,富含G和C的单链在生理条件下均形成发夹。富含C的链比富含G的链的发夹形成倾向更明显。该观察结果表明,富含C的链更可能形成发夹或“滑移”结构,并在复制过程中显示出不对称的链膨胀。 NMR数据还显示,富C链形成的发夹折叠的方式是茎的CpG步骤处的胞嘧啶为C.C配对。 CpG位点存在C.C不匹配会产生局部柔性,从而提供向甲基转移酶过渡的类似物。换句话说,富C链的发夹比Watson-Crick双链体或G富链的人甲基转移酶更好。因此,发夹形成可以解释在疾病发作期间在FMR1基因失活期间发生的脆弱X重复中CpG岛的特异性甲基化。

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