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首页> 外文期刊>Journal of Molecular Biology >Unpaired Structures in SCA10 (ATTCT)(n).(AGAAT)(n) Repeats.
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Unpaired Structures in SCA10 (ATTCT)(n).(AGAAT)(n) Repeats.

机译:SCA10中的未配对结构(ATTCT)(n)。(AGAAT)(n)重复。

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摘要

A number of human hereditary diseases have been associated with the instability of DNA repeats in the genome. Recently, spinocerebellar ataxia type 10 has been associated with expansion of the pentanucleotide repeat (ATTCT)(n).(AGAAT)(n) from a normal range of ten to 22 to as many as 4500 copies. The structural properties of this repeat cloned in circular plasmids were studied by a variety of methods. Two-dimensional gel electrophoresis and atomic force microscopy detected local DNA unpairing in supercoiled plasmids. Chemical probing analysis indicated that, at moderate superhelical densities, the (ATTCT)(n).(AGAAT)(n) repeat forms an unpaired region, which further extends into adjacent A+T-rich flanking sequences at higher superhelical densities. The superhelical energy required to initiate duplex unpairing is essentially length-independent from eight to 46 repeats. In plasmids containing five repeats, minimal unpairing of (ATTCT)(5).(AGAAT)(5) occurred while 2D gel analysis and chemical probing indicate greater unpairing in A+T-rich sequences in other regions of the plasmid. The observed experimental results are consistent with a statistical mechanical, computational analysis of these supercoiled plasmids. For plasmids containing 29 repeats, which is just above the normal human size range, flanked by an A+T-rich sequence, atomic force microscopy detected the formation of a locally condensed structure at high superhelical densities. However, even at high superhelical densities, DNA strands within the presumably compact A+T-rich region were accessible to small chemicals and oligonucleotide hybridization. Thus, DNA strands in this "collapsed structure" remain unpaired and accessible for interaction with other molecules. The unpaired DNA structure functioned as an aberrant replication origin, in that it supported complete plasmid replication in a HeLa cell extract. A model is proposed in which unscheduled or aberrant DNA replication is a critical step in the expansion mutation.
机译:许多人类遗传性疾病与基因组中DNA重复序列的不稳定性有关。最近,10型脊髓小脑共济失调与五核苷酸重复序列(ATTCT)(n)。(AGAAT)(n)的扩增范围从正常的10到22到多达4500个拷贝有关。通过多种方法研究了克隆在环状质粒中的该重复序列的结构特性。二维凝胶电泳和原子力显微镜检测到超螺旋质粒中的局部DNA不配对。化学探测分析表明,在中等超螺旋密度下,(ATTCT)(n)。(AGAAT)(n)重复序列会形成一个不成对区域,并以更高的超螺旋密度进一步延伸到相邻的富含A + T的侧翼序列中。启动双链不配对所需的超螺旋能量基本上与长度无关,从8个重复到46个重复。在含有5个重复序列的质粒中,(ATTCT)(5)。(AGAAT)(5)的最小不配对发生,而2D凝胶分析和化学探测表明在质粒其他区域中富含A + T的序列中更大的不配对。观察到的实验结果与这些超螺旋质粒的统计机械计算分析是一致的。对于含有29个重复序列的质粒,该序列刚好超出正常人的大小范围,侧翼是富含A + T的序列,原子力显微镜检测到了在超超高螺旋密度下局部浓缩结构的形成。然而,即使在高超螺旋密度下,假定的紧密的富含A + T的区域内的DNA链也可以通过小化学试剂和寡核苷酸杂交获得。因此,这种“折叠结构”中的DNA链保持不成对且可与其他分子相互作用。未配对的DNA结构起异常复制起点的作用,因为它支持HeLa细胞提取物中的完整质粒复制。提出了一种模型,其中计划外或异常的DNA复制是扩增突变中的关键步骤。

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