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DNA compaction by the bacteriophage protein Cox studied on the single DNA molecule level using nanofluidic channels

机译:使用纳米流体通道在单个DNA分子水平上研究了噬菌体蛋白Cox对DNA的致密作用

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摘要

The Cox protein from bacteriophage P2 forms oligomeric filaments and it has been proposed that DNA can be wound up around these filaments, similar to how histones condense DNA. We here use fluorescence microscopy to study single DNA–Cox complexes in nanofluidic channels and compare how the Cox homologs from phages P2 and WΦ affect DNA. By measuring the extension of nanoconfined DNA in absence and presence of Cox we show that the protein compacts DNA and that the binding is highly cooperative, in agreement with the model of a Cox filament around which DNA is wrapped. Furthermore, comparing microscopy images for the wild-type P2 Cox protein and two mutants allows us to discriminate between compaction due to filament formation and compaction by monomeric Cox. P2 and WΦ Cox have similar effects on the physical properties of DNA and the subtle, but significant, differences in DNA binding are due to differences in binding affinity rather than binding mode. The presented work highlights the use of single DNA molecule studies to confirm structural predictions from X-ray crystallography. It also shows how a small protein by oligomerization can have great impact on the organization of DNA and thereby fulfill multiple regulatory functions.
机译:来自噬菌体P2的Cox蛋白形成寡聚体细丝,有人提出DNA可以缠绕在这些细丝周围,类似于组蛋白如何凝结DNA。我们在这里使用荧光显微镜研究纳米流体通道中的单个DNA–Cox复合物,并比较噬菌体P2和WΦ中的Cox同源物如何影响DNA。通过在不存在和存在Cox的情况下测量纳米约束DNA的延伸,我们证明了该蛋白能紧实DNA,并且结合高度协作,这与包裹DNA的Cox细丝的模型一致。此外,比较野生型P2 Cox蛋白和两个突变体的显微图像,可以区分细丝形成引起的压实和单体Cox的压实。 P2和WΦCox对DNA和微妙的物理性质具有相似的影响,但是DNA结合的显着差异是由于结合亲和力而不是结合方式的差异。提出的工作强调了使用单个DNA分子研究来确认X射线晶体学的结构预测。它还显示了通过寡聚作用产生的小蛋白质如何对DNA的组织产生巨大影响,从而实现多种调节功能。

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