III-A 型 CRISPR 相关蛋白 Csm3 的结构与 RNA 结合特性。
Structure and RNA-binding properties of the type III-A CRISPR-associated protein Csm3.
机构信息
Structural Cell Biology Department; Max Planck Institute of Biochemistry; Munich/Martinsried, Germany.
Max Planck Institute for Terrestrial Microbiology; Karl-von-Frisch-Straße 10, Marburg, Germany.
出版信息
RNA Biol. 2013 Nov;10(11):1670-8. doi: 10.4161/rna.26500. Epub 2013 Sep 30.
Abstract
The prokaryotic adaptive immune system is based on the incorporation of genome fragments of invading viral genetic elements into clusters of regulatory interspaced short palindromic repeats (CRISPRs). The CRISPR loci are transcribed and processed into crRNAs, which are then used to target the invading nucleic acid for degradation. The large family of CRISPR-associated (Cas) proteins mediates this interference response. We have characterized Methanopyrus kandleri Csm3, a protein of the type III-A CRISPR-Cas complex. The 2.4 Å resolution crystal structure shows an elaborate four-domain fold organized around a core RRM-like domain. The overall architecture highlights the structural homology to Cas7, the Cas protein that forms the backbone of type I interference complexes. Csm3 binds unstructured RNAs in a sequence non-specific manner, suggesting that it interacts with the variable spacer sequence of the crRNA. The structural and biochemical data provide insights into the similarities and differences in this group of Cas proteins.
摘要
原核适应性免疫系统基于将入侵病毒遗传元件的基因组片段整合到调控间隔短回文重复序列 (CRISPRs) 的簇中。CRISPR 基因座被转录并加工成 crRNA,然后用于靶向入侵核酸进行降解。大量的 CRISPR 相关 (Cas) 蛋白介导这种干扰反应。我们已经对 Methanopyrus kandleri Csm3 进行了表征,这是一种 III-A 型 CRISPR-Cas 复合物的蛋白质。2.4 Å 分辨率的晶体结构显示了一种精心设计的四结构域折叠,围绕一个核心 RRM 样结构域组织。整体结构突出了与 Cas7 的结构同源性,Cas7 是构成 I 型干扰复合物骨架的 Cas 蛋白。Csm3 以非序列特异性的方式结合无结构的 RNA,表明它与 crRNA 的可变间隔序列相互作用。结构和生化数据提供了对这组 Cas 蛋白相似性和差异的深入了解。
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