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MCM解旋酶与DNA相互作用的原子力显微镜研究

Atomic Force Microscopy Investigation of the Interactions between the MCM Helicase and DNA.

作者信息

Mohammed Khalid Amna Abdalla, Parisse Pietro, Medagli Barbara, Onesti Silvia, Casalis Loredana

机构信息

Elettra-Sincrotrone Trieste, 34149 Trieste, Italy.

Department of Physics, PhD School in Nanotechnology, University of Trieste, 34127 Trieste, Italy.

出版信息

Materials (Basel). 2021 Feb 2;14(3):687. doi: 10.3390/ma14030687.

Abstract

The MCM (minichromosome maintenance) protein complex forms an hexameric ring and has a key role in the replication machinery of Eukaryotes and Archaea, where it functions as the replicative helicase opening up the DNA double helix ahead of the polymerases. Here, we present a study of the interaction between DNA and the archaeal MCM complex from by means of atomic force microscopy (AFM) single molecule imaging. We first optimized the protocol (surface treatment and buffer conditions) to obtain AFM images of surface-equilibrated DNA molecules before and after the interaction with the protein complex. We discriminated between two modes of interaction, one in which the protein induces a sharp bend in the DNA, and one where there is no bending. We found that the presence of the MCM complex also affects the DNA contour length. A possible interpretation of the observed behavior is that in one case the hexameric ring encircles the dsDNA, while in the other the nucleic acid wraps on the outside of the ring, undergoing a change of direction. We confirmed this topographical assignment by testing two mutants, one affecting the N-terminal β-hairpins projecting towards the central channel, and thus preventing DNA loading, the other lacking an external subdomain and thus preventing wrapping. The statistical analysis of the distribution of the protein complexes between the two modes, together with the dissection of the changes of DNA contour length and binding angle upon interaction, for the wild type and the two mutants, is consistent with the hypothesis. We discuss the results in view of the various modes of nucleic acid interactions that have been proposed for both archaeal and eukaryotic MCM complexes.

摘要

微小染色体维持(MCM)蛋白复合体形成一个六聚体环,在真核生物和古细菌的复制机制中起关键作用,它作为复制解旋酶在聚合酶之前打开DNA双螺旋。在此,我们通过原子力显微镜(AFM)单分子成像研究了DNA与来自[具体来源未给出]的古细菌MCM复合体之间的相互作用。我们首先优化了实验方案(表面处理和缓冲条件),以获得与蛋白质复合体相互作用前后表面平衡的DNA分子的AFM图像。我们区分了两种相互作用模式,一种是蛋白质使DNA产生急剧弯曲,另一种则没有弯曲。我们发现MCM复合体的存在也会影响DNA的轮廓长度。对观察到的行为的一种可能解释是,在一种情况下六聚体环环绕双链DNA,而在另一种情况下核酸缠绕在环的外部,方向发生改变。我们通过测试两个突变体证实了这种拓扑结构的归属,一个突变体影响向中央通道突出的N端β发夹结构,从而阻止DNA加载,另一个缺乏外部亚结构域,从而阻止缠绕。对野生型和两个突变体在两种模式之间蛋白质复合体分布的统计分析,以及对相互作用时DNA轮廓长度和结合角度变化的剖析,都与该假设一致。我们根据针对古细菌和真核生物MCM复合体提出的核酸相互作用的各种模式来讨论这些结果。

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