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真核转座子中的简单拓扑过滤器作为抑制基因组不稳定性的机制。

A simple topological filter in a eukaryotic transposon as a mechanism to suppress genome instability.

机构信息

School of Biomedical Sciences, University of Nottingham, Queen's Medical Centre, Nottingham NG7 2UH, United Kingdom.

出版信息

Mol Cell Biol. 2011 Jan;31(2):317-27. doi: 10.1128/MCB.01066-10. Epub 2010 Nov 1.

Abstract

DNA transposition takes place within a higher-order complex known as the transpososome. Almost everything known about its assembly has been gleaned from bacterial transposons. Here we present a detailed analysis of transpososome assembly in the human Hsmar1 element. The transpososome is nominally symmetrical, consisting of two identical transposon ends and a dimer of transposase. However, after the transposase dimer has captured the first transposon end, an asymmetry is introduced, raising a barrier against recruitment of the second end. The barrier can be overcome by right-handed plectonemic intertwining of the transposon ends. This likely occurs mainly during transcription and episodes of nucleosome remodeling. Plectonemic intertwining favors only synapsis of closely linked transposon ends in the inverted-repeat configuration and therefore suppresses the promiscuous synapsis of distant transposon ends, which initiate McClintock's chromosomal breakage-fusion-bridge cycles in maize. We also show that synapsis of the transposon ends is a prerequisite for the first catalytic step. This provides constraints on the enzymatic mechanism of the double-strand breaks in mariner transposition, excluding the most prevalent of the current models.

摘要

DNA 转座发生在一个被称为转座体的高级复合物中。人们对其组装的几乎所有了解都来自于细菌转座子。在这里,我们对人类 Hsmar1 元件中转座体的组装进行了详细分析。转座体是名义上对称的,由两个相同的转座子末端和转座酶二聚体组成。然而,在转座酶二聚体捕获第一个转座子末端后,会引入不对称性,从而对第二个末端的招募形成障碍。该障碍可以通过转座子末端的右手螺旋缠绕来克服。这种情况可能主要发生在转录和核小体重塑过程中。螺旋缠绕只有利于紧密连接的反向重复配置中转座子末端的联会,因此抑制了远距离转座子末端的随意联会,而这种联会启动了玉米中 McClintock 的染色体断裂-融合-桥循环。我们还表明,转座子末端的联会是第一个催化步骤的前提条件。这对 mariner 转座中的双链断裂的酶促机制施加了限制,排除了当前最流行的模型。

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