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首页> 外文期刊>Nucleic Acids Research >A novel immunity system for bacterial nucleic acid degrading toxins and its recruitment in various eukaryotic and DNA viral systems
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A novel immunity system for bacterial nucleic acid degrading toxins and its recruitment in various eukaryotic and DNA viral systems

机译:细菌核酸降解毒素的新型免疫系统及其在各种真核和DNA病毒系统中的募集

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摘要

The use of nucleases as toxins for defense, offense or addiction of selfish elements is widely encountered across all life forms. Using sensitive sequence profile analysis methods, we characterize a novel superfamily (the SUKH superfamily) that unites a diverse group of proteins including Smi1/Knr4, PGs2, FBXO3, SKIP16, Syd, herpesviral US22, IRS1 and TRS1, and their bacterial homologs. Using contextual analysis we present evidence that the bacterial members of this superfamily are potential immunity proteins for a variety of toxin systems that also include the recently characterized contact-dependent inhibition (CDI) systems of proteobacteria. By analyzing the toxin proteins encoded in the neighborhood of the SUKH superfamily we predict that they possess domains belonging to diverse nuclease and nucleic acid deaminase families. These include at least eight distinct types of DNases belonging to HNH/EndoVII- and restriction endonuclease-fold, and RNases of the EndoU-like and colicin E3-like cytotoxic RNases-folds. The N-terminal domains of these toxins indicate that they are extruded by several distinct secretory mechanisms such as the two-partner system (shared with the CDI systems) in proteobacteria, ESAT-6/WXG-like ATP-dependent secretory systems in Gram-positive bacteria and the conventional Sec-dependent system in several bacterial lineages. The hedgehog-intein domain might also release a subset of toxic nuclease domains through auto-proteolytic action. Unlike classical colicin-like nuclease toxins, the overwhelming majority of toxin systems with the SUKH superfamily is chromosomally encoded and appears to have diversified through a recombination process combining different C-terminal nuclease domains to N-terminal secretion-related domains. Across the bacterial superkingdom these systems might participate in discriminating `self' or kin from `non-self' or non-kin strains. Using structural analysis we demonstrate that the SUKH domain possesses a versatile scaffold that can be used to bind a wide range of protein partners. In eukaryotes it appears to have been recruited as an adaptor to regulate modification of proteins by ubiquitination or polyglutamylation. Similarly, another widespread immunity protein from these toxin systems, namely the suppressor of fused (SuFu) superfamily has been recruited for comparable roles in eukaryotes. In animal DNA viruses, such as herpesviruses, poxviruses, iridoviruses and adenoviruses, the ability of the SUKH domain to bind diverse targets has been deployed to counter diverse anti-viral responses by interacting with specific host proteins.
机译:在所有生命形式中,广泛使用核酸酶作为防御,进攻或自私成瘾的毒素。使用敏感的序列概况分析方法,我们表征了一个新的超家族(SUKH超家族),该家族结合了多种蛋白质,包括Smi1 / Knr4,PGs2,FBXO3,SKIP16,Syd,疱疹病毒US22,IRS1和TRS1及其细菌同源物。使用上下文分析,我们提供证据表明,该超家族的细菌成员是多种毒素系统的潜在免疫蛋白,其中还包括最近表征的变形细菌的接触依赖性抑制(CDI)系统。通过分析SUKH超家族附近编码的毒素蛋白,我们预测它们具有属于不同核酸酶和核酸脱氨酶家族的域。这些包括属于HNH / EndoVII和限制性核酸内切酶折叠的至少八种不同类型的DNase,以及EndoU样和大肠菌素E3样细胞毒性RNase折叠的RNase。这些毒素的N末端结构域表明它们是由几种不同的分泌机制(如蛋白细菌中的两伙伴系统(与CDI系统共享),ESAT-6 / WXG样的ATP依赖性分泌系统)挤出的。阳性细菌和几个细菌谱系中的常规Sec依赖性系统。刺猬蛋白内在结构域还可能通过自身蛋白水解作用释放出一部分毒性核酸酶结构域。与经典的大肠菌素样核酸酶毒素不同,具有SUKH超家族的绝大多数毒素系统是染色体编码的,并且似乎通过重组过程实现了多样化,该重组过程将不同的C端核酸酶结构域与N端分泌相关结构域结合在一起。在整个细菌超级王国中,这些系统可能参与将“自我”或亲属与“非自我”或非亲属菌株区分开来。使用结构分析,我们证明SUKH结构域具有通用的支架,可用于结合多种蛋白伴侣。在真核生物中,它似乎已被招募为通过泛素化或聚谷氨酰化来调节蛋白质修饰的衔接子。同样,已经从这些毒素系统中获得了另一种广泛的免疫蛋白,即融合(SuFu)超家族的抑制剂,以在真核生物中发挥类似作用。在动物DNA病毒(例如疱疹病毒,痘病毒,虹膜病毒和腺病毒)中,SUKH域结合多种靶标的能力已被部署来通过与特定宿主蛋白相互作用来抵抗多种抗病毒反应。

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