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Csm2 和 Csm3 在 III-A 型 CRISPR-Cas 效应复合物中的晶体结构。

Crystal Structures of Csm2 and Csm3 in the Type III-A CRISPR-Cas Effector Complex.

机构信息

Biomedical Research Institute, National Institute of Advanced Industrial Science and Technology (AIST), 1-1-1 Higashi, Tsukuba-shi, Ibaraki 305-8566, Japan.

Biomedical Research Institute, National Institute of Advanced Industrial Science and Technology (AIST), 1-1-1 Higashi, Tsukuba-shi, Ibaraki 305-8566, Japan.

出版信息

J Mol Biol. 2019 Feb 15;431(4):748-763. doi: 10.1016/j.jmb.2019.01.009. Epub 2019 Jan 11.

Abstract

Clustered regularly interspaced short palindromic repeat (CRISPR) loci and CRISPR-associated (Cas) genes encode CRISPR RNAs (crRNA) and Cas proteins, respectively, which play important roles in the adaptive immunity system (CRISPR-Cas system) in prokaryotes. The crRNA and Cas proteins form ribonucleoprotein effector complexes to capture and degrade invading genetic materials with base complementarity to the crRNA guide sequences. The Csm complex, a type III-A effector complex, comprises five Cas proteins (Csm1-Csm5) and a crRNA, which co-transcriptionally degrades invading DNA and RNA. Here we report the crystal structures of the Staphylococcus epidermidis Csm2 (SeCsm2) and Thermoplasma volcanium Csm3 (TvCsm3) at 2.4- and 2.7-Å resolutions, respectively. SeCsm2 adopts a monomeric globular fold by itself, in striking contrast to the previously reported Thermotoga maritima Csm2, which adopted an extended conformation and formed a dimeric structure. We propose that the globular monomeric form is the bona fide structure of Csm2. TvCsm3 forms a filamentous structure in the crystals. The molecular arrangement of TvCsm3 is similar to that of the stacked Cmr4 proteins in the Cmr complex, suggesting the functionally relevant architecture of the present Csm3 structure. We constructed model structures of the Csm complex, which revealed that Csm3 binds the crRNA and periodically deforms the crRNA-target duplex by a similar mechanism to that of Cmr4 in the Cmr complex. The model and mutational analysis suggest that the conserved lysine residue of Csm2 is important for target RNA binding, and Csm2 stabilizes the active structure of the Csm complex to facilitate the reaction.

摘要

成簇规律间隔短回文重复(CRISPR)基因座和 CRISPR 相关(Cas)基因分别编码 CRISPR RNA(crRNA)和 Cas 蛋白,它们在原核生物的适应性免疫系统(CRISPR-Cas 系统)中发挥重要作用。crRNA 和 Cas 蛋白形成核糖核蛋白效应复合物,以捕获和降解与 crRNA 指导序列具有碱基互补性的入侵遗传物质。Csm 复合物是一种 III-A 型效应复合物,由五个 Cas 蛋白(Csm1-Csm5)和一个 crRNA 组成,共同转录降解入侵的 DNA 和 RNA。在这里,我们报告了葡萄球菌表皮 Csm2(SeCsm2)和火球菌 Csm3(TvCsm3)的晶体结构,分辨率分别为 2.4 和 2.7Å。SeCsm2 自身采用单体球状折叠,与先前报道的海洋栖热菌 Csm2 形成延伸构象并形成二聚体结构形成鲜明对比。我们提出球状单体形式是 Csm2 的真实结构。TvCsm3 在晶体中形成丝状结构。TvCsm3 的分子排列与 Cmr 复合物中堆叠的 Cmr4 蛋白相似,表明目前 Csm3 结构具有功能相关的结构。我们构建了 Csm 复合物的模型结构,该结构揭示了 Csm3 通过类似于 Cmr 复合物中 Cmr4 的机制结合 crRNA 并周期性地使 crRNA-靶双链体变形。模型和突变分析表明,Csm2 的保守赖氨酸残基对于靶 RNA 结合很重要,并且 Csm2 稳定 Csm 复合物的活性结构以促进反应。

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