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Microscopic mechanism of DNA damage searching by hOGG1

机译:Hogg1搜索DNA损伤的显微镜机制

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摘要

The DNA backbone is often considered a track that allows long-range sliding of DNA repair enzymes in their search for rare damage sites in DNA. A proposed exemplar of DNA sliding is human 8-oxoguanine ((o)G) DNA glycosylase 1 (hOGG1), which repairs mutagenic (o)G lesions in DNA. Here we use our high-resolution molecular clock method to show that macroscopic 1D DNA sliding of hOGG1 occurs by microscopic 2D and 3D steps that masquerade as sliding in resolution-limited single-molecule images. Strand sliding was limited to distances shorter than seven phosphate linkages because attaching a covalent chemical road block to a single DNA phosphate located between two closely spaced damage sites had little effect on transfers. The microscopic parameters describing the DNA search of hOGG1 were derived from numerical simulations constrained by the experimental data. These findings support a general mechanism where DNA glycosylases use highly dynamic-multidimensional diffusion paths to scan DNA.
机译:DNA骨架通常被认为是允许DNA修复酶的远程滑动在他们寻找DNA中的罕见损伤部位。 DNA滑动的提出示例是人8-氧代((O)G)DNA糖基糖基酶1(术HogG1),其在DNA中修复诱变(O)G病变。 在这里,我们使用我们的高分辨率分子时钟方法来表明Hogg1的宏观1D DNA滑动通过微观的2D和3D步骤,使伪装成在分辨率限制的单分子图像中滑动。 股线滑动仅限于短于七个磷酸盐键的距离,因为将共价化学路嵌段连接到位于两个紧密间隔的损伤部位之间的单个DNA磷酸盐对转移几乎没有影响。 描述霍格1的DNA搜索的微观参数源自由实验数据约束的数值模拟。 这些发现支持一种通用机制,其中DNA糖基团使用高动态多维扩散路径来扫描DNA。

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