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DUF2285 是一种新型的螺旋-转角-螺旋结构域变体,可协调变形菌中接合元件转移的激活和拮抗作用。

DUF2285 is a novel helix-turn-helix domain variant that orchestrates both activation and antiactivation of conjugative element transfer in proteobacteria.

机构信息

Department of Microbiology and Immunology, University of Otago, Dunedin 9016, New Zealand.

School of Molecular Sciences, University of Western Australia, 35 Stirling Highway, Crawley, WA 6009, Australia.

出版信息

Nucleic Acids Res. 2023 Jul 21;51(13):6841-6856. doi: 10.1093/nar/gkad457.

Abstract

Horizontal gene transfer is tightly regulated in bacteria. Often only a fraction of cells become donors even when regulation of horizontal transfer is coordinated at the cell population level by quorum sensing. Here, we reveal the widespread 'domain of unknown function' DUF2285 represents an 'extended-turn' variant of the helix-turn-helix domain that participates in both transcriptional activation and antiactivation to initiate or inhibit horizontal gene transfer. Transfer of the integrative and conjugative element ICEMlSymR7A is controlled by the DUF2285-containing transcriptional activator FseA. One side of the DUF2285 domain of FseA has a positively charged surface which is required for DNA binding, while the opposite side makes critical interdomain contacts with the N-terminal FseA DUF6499 domain. The QseM protein is an antiactivator of FseA and is composed of a DUF2285 domain with a negative surface charge. While QseM lacks the DUF6499 domain, it can bind the FseA DUF6499 domain and prevent transcriptional activation by FseA. DUF2285-domain proteins are encoded on mobile elements throughout the proteobacteria, suggesting regulation of gene transfer by DUF2285 domains is a widespread phenomenon. These findings provide a striking example of how antagonistic domain paralogues have evolved to provide robust molecular control over the initiation of horizontal gene transfer.

摘要

水平基因转移在细菌中受到严格调控。即使在群体水平上通过群体感应协调水平转移的调控,通常也只有一小部分细胞成为供体。在这里,我们揭示了广泛存在的“未知功能域”DUF2285 代表了螺旋-转角-螺旋结构域的“扩展转角”变体,该结构域参与转录激活和反激活,以启动或抑制水平基因转移。整合和共轭元件 ICEMlSymR7A 的转移受包含 DUF2285 的转录激活因子 FseA 控制。FseA 的 DUF2285 结构域的一侧具有带正电荷的表面,这是 DNA 结合所必需的,而另一侧与 FseA 的 N 端 DUF6499 结构域形成关键的结构域间接触。QseM 蛋白是 FseA 的反激活因子,由带负电荷表面的 DUF2285 结构域组成。虽然 QseM 缺乏 DUF6499 结构域,但它可以结合 FseA 的 DUF6499 结构域并阻止 FseA 的转录激活。DUF2285 结构域蛋白编码在整个变形菌门的移动元件上,这表明 DUF2285 结构域对基因转移的调控是一种广泛存在的现象。这些发现为 DUF2285 结构域如何进化为提供对水平基因转移起始的强大分子控制提供了一个惊人的例子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ddf4/10359603/ea2133778504/gkad457figgra1.jpg

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