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Human DNA polymerase α in binary complex with a DNA:DNA template-primer

机译:人类DNA聚合酶α与DNA:DNA模板引物二元复合物

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摘要

The Polα/primase complex assembles the short RNA-DNA fragments for priming of lagging and leading strand DNA replication in eukaryotes. As such, the Polα polymerase subunit encounters two types of substrates during primer synthesis: an RNA:DNA helix and a DNA:DNA helix. The engagement of the polymerase subunit with the DNA:DNA helix has been suggested as the of basis for primer termination in eukaryotes. However, there is no structural information on how the Polα polymerase subunit actually engages with a DNA:DNA helix during primer synthesis. We present here the first crystal structure of human Polα polymerase subunit in complex with a DNA:DNA helix. Unexpectedly, we find that portion of the DNA:DNA helix in contact with the polymerase is not in a B-form but in a hybrid A-B form. Almost all of the contacts observed previously with an RNA primer are preserved with a DNA primer--with the same set of polymerase residues tracking the sugar-phosphate backbone of the DNA or RNA primer. Thus, rather than loss of specific contacts, the free energy cost of distorting DNA from B- to hybrid A-B form may augur the termination of primer synthesis in eukaryotes.
机译:Polα/引发酶复合物组装短的RNA-DNA片段,用于引发真核生物中滞后和前导链DNA复制。这样,Polα聚合酶亚基在引物合成过程中会遇到两种类型的底物:RNA:DNA螺旋和DNA:DNA螺旋。已经提出聚合酶亚基与DNA:DNA螺旋的结合作为真核生物中引物终止的基础。但是,没有关于引物合成过程中Polα聚合酶亚基实际上如何与DNA:DNA螺旋结合的结构信息。我们在这里展示了人类Polα聚合酶亚基与DNA:DNA螺旋复合的第一个晶体结构。出乎意料的是,我们发现与聚合酶接触的DNA:DNA螺旋部分不是B形式而是杂种A-B形式。以前用RNA引物观察到的几乎所有接触都用DNA引物保存-具有追踪DNA或RNA引物的糖磷酸骨架的同一组聚合酶残基。因此,将DNA从B-形式变形为杂种A-B形式而不是失去特定的接触,可能会使真核生物中引物合成终止的自由能成本增加。

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