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Co-evolution of quaternary organization and novel RNA tertiary interactions revealed in the crystal structure of a bacterial protein–RNA toxin–antitoxin system

机译:细菌蛋白-RNA毒素-抗毒素系统的晶体结构揭示了四级组织和新的RNA三级相互作用的共同进化

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摘要

Genes encoding toxin–antitoxin (TA) systems are near ubiquitous in bacterial genomes and they play key roles in important aspects of bacterial physiology, including genomic stability, formation of persister cells under antibiotic stress, and resistance to phage infection. The CptIN locus from Eubacterium rectale is a member of the recently-discovered Type III class of TA systems, defined by a protein toxin suppressed by direct interaction with a structured RNA antitoxin. Here, we present the crystal structure of the CptIN protein–RNA complex to 2.2 Å resolution. The structure reveals a new heterotetrameric quaternary organization for the Type III TA class, and the RNA antitoxin bears a novel structural feature of an extended A-twist motif within the pseudoknot fold. The retention of a conserved ribonuclease active site as well as traits normally associated with TA systems, such as plasmid maintenance, implicates a wider functional role for Type III TA systems. We present evidence for the co-variation of the Type III component pair, highlighting a distinctive evolutionary process in which an enzyme and its substrate co-evolve.
机译:编码毒素-抗毒素(TA)系统的基因在细菌基因组中几乎无处不在,它们在细菌生理学的重要方面起着关键作用,包括基因组稳定性,在抗生素胁迫下形成持久性细胞以及对噬菌体感染的抵抗力。来自直肠真细菌的CptIN基因座是最近发现的TA系统的III类成员,其定义为通过与结构化RNA抗毒素直接相互作用而被抑制的蛋白毒素。在这里,我们介绍了CptIN蛋白-RNA复合物的晶体结构,分辨率为2.2Å。该结构揭示了III型TA类的新的异四聚体四级结构,RNA抗毒素具有假结折叠内扩展的A扭曲基序的新结构特征。保守的核糖核酸酶活性位点的保留以及通常与TA系统相关的性状,例如质粒的维持,对III型TA系统具有更广泛的功能。我们为类型III组件对的共变提供了证据,突出了酶及其底物共同进化的独特进化过程。

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