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热稳定 RecQ 样解旋酶和拓扑异构酶 3 蛋白在霍利迪连接体加工和复制叉稳定中的协同和拮抗作用。

Synergic and opposing activities of thermophilic RecQ-like helicase and topoisomerase 3 proteins in Holliday junction processing and replication fork stabilization.

机构信息

Institute of Protein Biochemistry, Consiglio Nazionale delle Ricerche, Via P. Castellino 111, 80131 Naples, Italy.

出版信息

J Biol Chem. 2012 Aug 31;287(36):30282-95. doi: 10.1074/jbc.M112.366377. Epub 2012 Jun 21.

Abstract

RecQ family helicases and topoisomerase 3 enzymes form evolutionary conserved complexes that play essential functions in DNA replication, recombination, and repair, and in vitro, show coordinate activities on model recombination and replication intermediates. Malfunctioning of these complexes in humans is associated with genomic instability and cancer-prone syndromes. Although both RecQ-like and topoisomerase 3 enzymes are present in archaea, only a few of them have been studied, and no information about their functional interaction is available. We tested the combined activities of the RecQ-like helicase, Hel112, and the topoisomerase 3, SsTop3, from the thermophilic archaeon Sulfolobus solfataricus. Hel112 showed coordinate DNA unwinding and annealing activities, a feature shared by eukaryotic RecQ homologs, which resulted in processing of synthetic Holliday junctions and stabilization of model replication forks. SsTop3 catalyzed DNA relaxation and annealing. When assayed in combination, SsTop3 inhibited the Hel112 helicase activity on Holliday junctions and stimulated formation and stabilization of such structures. In contrast, Hel112 did not affect the SsTop3 DNA relaxation activity. RecQ-topoisomerase 3 complexes show structural similarity with the thermophile-specific enzyme reverse gyrase, which catalyzes positive supercoiling of DNA and was suggested to play a role in genome stability at high temperature. Despite such similarity and the high temperature of reaction, the SsTop3-Hel112 complex does not induce positive supercoiling and is thus likely to play different roles. We propose that the interplay between Hel112 and SsTop3 might regulate the equilibrium between recombination and anti-recombination activities at replication forks.

摘要

RecQ 家族解旋酶和拓扑异构酶 3 酶形成进化上保守的复合物,在 DNA 复制、重组和修复中发挥重要功能,在体外,在模型重组和复制中间体上显示协调的活性。这些复合物在人类中的功能障碍与基因组不稳定性和癌症易患综合征有关。尽管古菌中存在 RecQ 样和拓扑异构酶 3 酶,但只有少数几种得到了研究,并且没有关于它们功能相互作用的信息。我们测试了嗜热古菌 Sulfolobus solfataricus 中的 RecQ 样解旋酶 Hel112 和拓扑异构酶 3 SsTop3 的联合活性。Hel112 显示出协调的 DNA 解旋和退火活性,这是真核 RecQ 同源物的特征,导致合成的 Holliday 连接点的处理和模型复制叉的稳定。SsTop3 催化 DNA 松弛和退火。当联合测定时,SsTop3 抑制 Hel112 解旋酶在 Holliday 连接点上的活性,并刺激此类结构的形成和稳定。相比之下,Hel112 不会影响 SsTop3 的 DNA 松弛活性。RecQ-拓扑异构酶 3 复合物与热原体特异性酶反转旋转酶具有结构相似性,反转旋转酶催化 DNA 的正超螺旋化,并被认为在高温下发挥稳定基因组的作用。尽管存在这种相似性和高温反应,但 SsTop3-Hel112 复合物不会诱导正超螺旋化,因此可能发挥不同的作用。我们提出,Hel112 和 SsTop3 之间的相互作用可能调节复制叉处重组和抗重组活性之间的平衡。

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