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串联甘氨酸核糖开关适体的不对称性和协同性。

The asymmetry and cooperativity of tandem glycine riboswitch aptamers.

机构信息

Chemical Biology Institute, Yale University, West Haven, Connecticut 06516, USA.

Department of Chemistry.

出版信息

RNA. 2020 May;26(5):564-580. doi: 10.1261/rna.073577.119. Epub 2020 Jan 28.

Abstract

Glycine riboswitches utilize both single- and tandem-aptamer architectures. In the tandem system, the relative contribution of each aptamer toward gene regulation is not well understood. To dissect these contributions, the effects of 684 single mutants of a tandem ON switch from were characterized for the wild-type construct and binding site mutations that selectively restrict ligand binding to either the first or second aptamer. Despite the structural symmetry of tandem aptamers, the response to these mutations was frequently asymmetrical. Mutations in the first aptamer often significantly weakened the , while several mutations in the second aptamer improved the amplitude. These results demonstrate that this ON switch favors ligand binding to the first aptamer. This is in contrast to the tandem OFF switch variant from , which was previously shown to have preferential binding to its second aptamer. A bioinformatic analysis of tandem glycine riboswitches revealed that the two binding pockets are differentially conserved between ON and OFF switches. Altogether, this indicates that tandem ON switch variants preferentially utilize binding to the first aptamer to promote helical switching, while OFF switch variants favor binding to the second aptamer. The data set also revealed a cooperative glycine response when both binding pockets were maximally stabilized with three GC base pairs. This indicates a cooperative response may sometimes be obfuscated by a difference in the affinities of the two aptamers. This conditional cooperativity provides an additional layer of tunability to tandem glycine riboswitches that adds to their versatility as genetic switches.

摘要

甘氨酰核糖开关利用单串联适体结构。在串联系统中,每个适体对基因调控的相对贡献尚不清楚。为了剖析这些贡献,我们对来自 的串联 ON 开关的 684 个单突变体的野生型构建体和结合位点突变体进行了特征描述,这些突变体选择性地限制配体与第一个或第二个适体结合。尽管串联适体在结构上是对称的,但这些突变的反应往往是不对称的。第一个适体的突变通常会显著削弱 ,而第二个适体的几个突变则提高了振幅。这些结果表明,这个 ON 开关有利于配体与第一个适体结合。这与来自 的串联 OFF 开关变体形成对比,先前的研究表明它优先与第二个适体结合。对串联甘氨酰核糖开关的生物信息学分析表明,两个结合口袋在 ON 和 OFF 开关之间的保守性存在差异。总的来说,这表明串联 ON 开关变体优先利用与第一个适体的结合来促进螺旋构象转换,而 OFF 开关变体则倾向于与第二个适体结合。该数据集还揭示了当两个结合口袋都通过三个 GC 碱基对最大程度地稳定化时,甘氨酸的协同反应。这表明,当两个适体的亲和力存在差异时,协同反应可能会变得模糊。这种条件协同性为串联甘氨酰核糖开关提供了额外的可调性,增加了它们作为遗传开关的多功能性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/24d2/7161355/893383c7a545/564f01.jpg

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