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CRISPRmap: an automated classification of repeat conservation in prokaryotic adaptive immune systems

机译:CRISPRmap:原核适应性免疫系统中重复保守的自动分类

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摘要

Central to Clustered Regularly Interspaced Short Palindromic Repeat (CRISPR)-Cas systems are repeated RNA sequences that serve as Cas-protein–binding templates. Classification is based on the architectural composition of associated Cas proteins, considering repeat evolution is essential to complete the picture. We compiled the largest data set of CRISPRs to date, performed comprehensive, independent clustering analyses and identified a novel set of 40 conserved sequence families and 33 potential structure motifs for Cas-endoribonucleases with some distinct conservation patterns. Evolutionary relationships are presented as a hierarchical map of sequence and structure similarities for both a quick and detailed insight into the diversity of CRISPR-Cas systems. In a comparison with Cas-subtypes, I-C, I-E, I-F and type II were strongly coupled and the remaining type I and type III subtypes were loosely coupled to repeat and Cas1 evolution, respectively. Subtypes with a strong link to CRISPR evolution were almost exclusive to bacteria; nevertheless, we identified rare examples of potential horizontal transfer of I-C and I-E systems into archaeal organisms. Our easy-to-use web server provides an automated assignment of newly sequenced CRISPRs to our classification system and enables more informed choices on future hypotheses in CRISPR-Cas research: .
机译:簇状规则间隔的短回文重复序列(CRISPR)-Cas系统的核心是重复的RNA序列,充当Cas蛋白结合模板。分类是基于相关Cas蛋白的结构组成,考虑重复进化对完成图片至关重要。我们收集了迄今为止最大的CRISPR数据集,进行了全面的独立聚类分析,并确定了40个保守序列家族和33个潜在的Cas-核糖核酸内切酶结构基序的新颖集合,并具有一些不同的保守模式。进化关系以序列和结构相似性的层次图的形式呈现,可以快速而详细地了解CRISPR-Cas系统的多样性。在与Cas亚型的比较中,I-C,I-E,I-F和II型紧密耦合,其余的I型和III型亚型分别松散耦合以重复和进行Cas1进化。与CRISPR进化有密切联系的亚型几乎是细菌所独有的。但是,我们发现了I-C和I-E系统潜在水平转移到古细菌中的罕见例子。我们易于使用的网络服务器将新测序的CRISPR自动分配给我们的分类系统,并为CRISPR-Cas研究中的未来假设提供更明智的选择:。

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