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CRISPR-Cas: Evolution of an RNA-based adaptive immunity system in prokaryotes

机译:CRISPR-Cas:原核生物中基于RNA的自适应免疫系统的进化

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The CRISPR-Cas (clustered regularly interspaced short palindromic repeats, CRISPR-associated genes) is an adaptive immunity system in bacteria and archaea that functions via a distinct self-non-self recognition mechanism that is partially analogous to the mechanism of eukaryotic RNA interference (RNAi). The CRISPR-Cas system incorporates fragments of virus or plasmid DNA into the CRISPR repeat cassettes and employs the processed transcripts of these spacers as guide RNAs to cleave the cognate foreign DNA or RNA. The Cas proteins, however, are not homologous to the proteins involved in RNAi and comprise numerous, highly diverged families. The majority of the Cas proteins contain diverse variants of the RNA recognition motif (RRM), a widespread RNA-binding domain. Despite the fast evolution that is typical of the cas genes, the presence of diverse versions of the RRM in most Cas proteins provides for a simple scenario for the evolution of the three distinct types of CRISPR-cas systems. In addition to several proteins that are directly implicated in the immune response, the cas genes encode a variety of proteins that are homologous to prokaryotic toxins that typically possess nuclease activity. The predicted toxins associated with CRISPR-Cas systems include the essential Cas2 protein, proteins of COG1517 that, in addition to a ligand-binding domain and a helix-turn-helix domain, typically contain different nuclease domains and several other predicted nucleases. The tight association of the CRISPR-Cas immunity systems with predicted toxins that, upon activation, would induce dormancy or cell death suggests that adaptive immunity and dormancy/suicide response are functionally coupled. Such coupling could manifest in the persistence state being induced and potentially providing conditions for more effective action of the immune system or in cell death being triggered when immunity fails.
机译:CRISPR-Cas(聚簇的规则间隔的短回文重复序列,与CRISPR相关的基因)是细菌和古细菌中的一种自适应免疫系统,通过独特的自我-非自我识别机制起作用,部分类似于真核RNA干扰机制( RNAi)。 CRISPR-Cas系统将病毒或质粒DNA片段整合到CRISPR重复盒中,并使用这些间隔子的加工转录本作为指导RNA裂解同源的外源DNA或RNA。但是,Cas蛋白与RNAi中涉及的蛋白并不同源,并且包含许多高度不同的家族。大多数Cas蛋白都包含RNA识别基序(RRM)(广泛的RNA结合结构域)的各种变体。尽管cas基因具有典型的快速进化,但大多数Cas蛋白中RRM的不同版本的存在为三种不同类型的CRISPR-cas系统的进化提供了简单的方案。除了直接参与免疫应答的几种蛋白质外,cas基因还编码与通常具有核酸酶活性的原核毒素同源的多种蛋白质。与CRISPR-Cas系统相关的预测毒素包括必需的Cas2蛋白,COG1517蛋白,除了配体结合结构域和螺旋-转-螺旋结构域外,还通常包含不同的核酸酶结构域和其他几种预测的核酸酶。 CRISPR-Cas免疫系统与预测的毒素紧密结合,该毒素在激活后会诱导休眠或细胞死亡,这表明适应性免疫和休眠/自杀反应在功能上是耦合的。这种耦合可以表现为持续状态的诱导,并可能为免疫系统的更有效作用提供条件,或者在免疫失败时触发细胞死亡。

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