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与双链 DNA 的碰撞使大肠埃希氏菌 DNA 聚合酶 III 全酶易受 DNA 聚合酶 IV 介导的滑动夹上聚合酶切换的影响。

Collision with duplex DNA renders Escherichia coli DNA polymerase III holoenzyme susceptible to DNA polymerase IV-mediated polymerase switching on the sliding clamp.

机构信息

Division of Systems Biology, Graduate School of Biological Sciences, Nara Institute of Science and Technology, Ikoma, Nara, 630-0192, Japan.

出版信息

Sci Rep. 2017 Oct 16;7(1):12755. doi: 10.1038/s41598-017-13080-1.

Abstract

Organisms possess multiple DNA polymerases (Pols) and use each for a different purpose. One of the five Pols in Escherichia coli, DNA polymerase IV (Pol IV), encoded by the dinB gene, is known to participate in lesion bypass at certain DNA adducts. To understand how cells choose Pols when the replication fork encounters an obstacle on template DNA, the process of polymerase exchange from the primary replicative enzyme DNA polymerase III (Pol III) to Pol IV was studied in vitro. Replicating Pol III forming a tight holoenzyme (Pol III HE) with the sliding clamp was challenged by Pol IV on a primed ssDNA template carrying a short inverted repeat. A rapid and lesion-independent switch from Pol III to Pol IV occurred when Pol III HE encountered a hairpin stem duplex, implying that the loss of Pol III-ssDNA contact induces switching to Pol IV. Supporting this idea, mutant Pol III with an increased affinity for ssDNA was more resistant to Pol IV than wild-type Pol III was. We observed that an exchange between Pol III and Pol IV also occurred when Pol III HE collided with primer/template duplex. Our data suggest that Pol III-ssDNA interaction may modulate the susceptibility of Pol III HE to Pol IV-mediated polymerase exchange.

摘要

生物体拥有多种 DNA 聚合酶(Pols),并将每种酶用于不同的目的。大肠杆菌中的五种 Pol 之一,即由 dinB 基因编码的 DNA 聚合酶 IV(Pol IV),已知参与特定 DNA 加合物的损伤绕过。为了了解细胞在复制叉遇到模板 DNA 上的障碍物时如何选择 Pols,我们在体外研究了从主要复制酶 DNA 聚合酶 III(Pol III)到 Pol IV 的聚合酶交换过程。复制 Pol III 与滑动夹形成紧密的全酶(Pol III HE),在带有短反向重复的引发 ssDNA 模板上受到 Pol IV 的挑战。当 Pol III HE 遇到发夹茎双链体时,会迅速发生与损伤无关的从 Pol III 到 Pol IV 的切换,这意味着 Pol III-ssDNA 接触的丧失会诱导向 Pol IV 的切换。支持这一观点的是,与 ssDNA 结合亲和力增加的突变型 Pol III 比野生型 Pol III 更能抵抗 Pol IV。我们观察到,当 Pol III HE 与引物/模板双链体碰撞时,Pol III 和 Pol IV 之间也会发生交换。我们的数据表明,Pol III-ssDNA 相互作用可能调节 Pol III HE 对 Pol IV 介导的聚合酶交换的敏感性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9a11/5643309/7f184d12c924/41598_2017_13080_Fig1_HTML.jpg

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