Anantharaman Vivek, Aravind L
National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health, Bethesda, MD 20894, USA.
Genome Biol. 2003;4(12):R81. doi: 10.1186/gb-2003-4-12-r81. Epub 2003 Nov 26.
Several prokaryotic plasmids maintain themselves in their hosts by means of diverse post-segregational cell killing systems. Recent findings suggest that chromosomally encoded copies of toxins and antitoxins of post-segregational cell killing systems - such as the RelE system - might function as regulatory switches under stress conditions. The RelE toxin cleaves ribosome-associated transcripts, whereas another post-segregational cell killing toxin, ParE, functions as a gyrase inhibitor.
Using sequence profile analysis we were able unify the RelE- and ParE-type toxins with several families of small, uncharacterized proteins from diverse bacteria and archaea into a single superfamily. Gene neighborhood analysis showed that the majority of these proteins were encoded by genes in characteristic neighborhoods, in which genes encoding toxins always co-occurred with genes encoding transcription factors that are also antitoxins. The transcription factors accompanying the RelE/ParE superfamily may belong to unrelated or distantly related superfamilies, however. We used this conserved neighborhood template to transitively search genomes and identify novel post-segregational cell killing-related systems. One of these novel systems, observed in several prokaryotes, contained a predicted toxin with a PilT-N terminal (PIN) domain, which is also found in proteins of the eukaryotic nonsense-mediated RNA decay system. These searches also identified novel transcription factors (antitoxins) in post-segregational cell killing systems. Furthermore, the toxin Doc defines a potential metalloenzyme superfamily, with novel representatives in bacteria, archaea and eukaryotes, that probably acts on nucleic acids.
The tightly maintained gene neighborhoods of post-segregational cell killing-related systems appear to have evolved by in situ displacement of genes for toxins or antitoxins by functionally equivalent but evolutionarily unrelated genes. We predict that the novel post-segregational cell killing-related systems containing a PilT-N terminal domain toxin and the eukaryotic nonsense-mediated RNA decay system are likely to function via a common mechanism, in which the PilT-N terminal domain cleaves ribosome-associated transcripts. The core of the eukaryotic nonsense-mediated RNA decay system has probably evolved from a post-segregational cell killing-related system.
几种原核生物质粒通过多种后分离细胞杀伤系统在宿主中维持自身。最近的研究结果表明,后分离细胞杀伤系统(如RelE系统)的毒素和抗毒素的染色体编码拷贝可能在应激条件下起调节开关的作用。RelE毒素切割核糖体相关转录本,而另一种后分离细胞杀伤毒素ParE则作为一种回旋酶抑制剂发挥作用。
通过序列谱分析,我们能够将RelE型和ParE型毒素与来自不同细菌和古菌的几个小的、未表征的蛋白质家族统一到一个单一的超家族中。基因邻域分析表明,这些蛋白质中的大多数由特征邻域中的基因编码,其中编码毒素的基因总是与编码也是抗毒素的转录因子的基因同时出现。然而,与RelE/ParE超家族相伴的转录因子可能属于不相关或远缘相关的超家族。我们使用这个保守的邻域模板来传递性地搜索基因组,并识别新的后分离细胞杀伤相关系统。在几种原核生物中观察到的这些新系统之一包含一种预测的具有PilT-N末端(PIN)结构域的毒素,这种结构域也存在于真核生物无义介导的RNA衰变系统的蛋白质中。这些搜索还在后分离细胞杀伤系统中识别出了新的转录因子(抗毒素)。此外,毒素Doc定义了一个潜在的金属酶超家族,在细菌、古菌和真核生物中有新的代表成员,可能作用于核酸。
后分离细胞杀伤相关系统紧密维持的基因邻域似乎是通过功能等效但进化上不相关的基因原位取代毒素或抗毒素基因而进化而来的。我们预测,包含PilT-N末端结构域毒素的新的后分离细胞杀伤相关系统和真核生物无义介导的RNA衰变系统可能通过共同机制发挥作用,其中PilT-N末端结构域切割核糖体相关转录本。真核生物无义介导的RNA衰变系统的核心可能是从后分离细胞杀伤相关系统进化而来的。
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