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当解旋酶和拓扑异构酶相遇时!

When helicase and topoisomerase meet!

作者信息

Duguet M

机构信息

Laboratoire d'Enzymologie des Acides Nucléiques, Institut de Génétique et Microbiologie, URA 2225 CNRS, Université Paris-Sud, Orsay, France.

出版信息

J Cell Sci. 1997 Jun;110 ( Pt 12):1345-50. doi: 10.1242/jcs.110.12.1345.

Abstract

Several examples of direct interactions between helicases and topoisomerases have recently been described. The data suggest a possible cooperation between these enzymes in major DNA events such as the progression of a replication fork, segregation of newly replicated chromosomes, disruption of nucleosomal structure, DNA supercoiling, and finally recombination, repair, and genomic stability. A first example is the finding of a strong interaction between T antigen and topoisomerase I in mammalian cells, that may trigger unwinding of the parental DNA strands at the replication forks of Simian Virus 40. A second example is the reverse gyrase from thermophilic prokaryotes, composed of a putative helicase domain, and a topoisomerase domain in the same polypeptide. This enzyme may be required to maintain genomic stability at high temperature. A third example is the finding of an interaction between type II topoisomerase and the helicase Sgs1 in yeast. This interaction possibly allows the faithful segregation of newly replicated chromosomes in eukaryotic cells. A fourth example is the interaction between the same helicase Sgs1 and topoisomerase III in yeast, that may control recombination level and genetic stability of repetitive sequences. Recently, in humans, mutations in genes similar to Sgs1 have been found to be responsible for Bloom's and Werner's syndromes. The cooperation between helicases and topoisomerases is likely to be extended to many aspects of DNA mechanisms including chromatin condensation/decondensation.

摘要

最近已经描述了解旋酶和拓扑异构酶之间直接相互作用的几个例子。数据表明,这些酶在主要的DNA事件中可能存在合作关系,如复制叉的推进、新复制染色体的分离、核小体结构的破坏、DNA超螺旋,以及最终的重组、修复和基因组稳定性。第一个例子是在哺乳动物细胞中发现T抗原与拓扑异构酶I之间存在强烈相互作用,这可能会引发猴病毒40复制叉处亲代DNA链的解旋。第二个例子是嗜热原核生物中的反向回旋酶,它由一个假定的解旋酶结构域和同一多肽中的一个拓扑异构酶结构域组成。这种酶可能是在高温下维持基因组稳定性所必需的。第三个例子是在酵母中发现II型拓扑异构酶与解旋酶Sgs1之间存在相互作用。这种相互作用可能使真核细胞中新复制的染色体得以准确分离。第四个例子是酵母中同一解旋酶Sgs1与拓扑异构酶III之间的相互作用,这可能控制重复序列的重组水平和遗传稳定性。最近,在人类中发现,与Sgs1相似的基因突变与布卢姆综合征和沃纳综合征有关。解旋酶和拓扑异构酶之间的合作可能会扩展到DNA机制的许多方面,包括染色质的凝聚/解凝聚。

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