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1
Tetramerisation of the CRISPR ring nuclease Crn3/Csx3 facilitates cyclic oligoadenylate cleavage.CRISPR环状核酸酶Crn3/Csx3的四聚化促进环状寡腺苷酸的切割。
Elife. 2020 Jun 29;9:e57627. doi: 10.7554/eLife.57627.
2
CBASS Immunity Uses CARF-Related Effectors to Sense 3'-5'- and 2'-5'-Linked Cyclic Oligonucleotide Signals and Protect Bacteria from Phage Infection.CBASS 免疫利用 CARF 相关效应子来感知 3'-5'-和 2'-5'-连接的环状寡核苷酸信号,并保护细菌免受噬菌体感染。
Cell. 2020 Jul 9;182(1):38-49.e17. doi: 10.1016/j.cell.2020.05.019. Epub 2020 Jun 15.
3
Fuse to defuse: a self-limiting ribonuclease-ring nuclease fusion for type III CRISPR defence.熔解来解除:III 型 CRISPR 防御的一种自我限制的核糖核酸酶-环核酶融合。
Nucleic Acids Res. 2020 Jun 19;48(11):6149-6156. doi: 10.1093/nar/gkaa298.
4
The dynamic interplay of host and viral enzymes in type III CRISPR-mediated cyclic nucleotide signalling.III 型 CRISPR 介导的环核苷酸信号中宿主和病毒酶的动态相互作用。
Elife. 2020 Apr 27;9:e55852. doi: 10.7554/eLife.55852.
5
Activation and self-inactivation mechanisms of the cyclic oligoadenylate-dependent CRISPR ribonuclease Csm6.环状寡腺苷酸依赖的 CRISPR 核糖核酸酶 Csm6 的激活和自我失活机制。
Nat Commun. 2020 Mar 27;11(1):1596. doi: 10.1038/s41467-020-15334-5.
6
Regulation of the RNA and DNA nuclease activities required for Pyrococcus furiosus Type III-B CRISPR-Cas immunity.火球菌属 III-B CRISPR-Cas 免疫所需的 RNA 和 DNA 核酸酶活性的调控。
Nucleic Acids Res. 2020 May 7;48(8):4418-4434. doi: 10.1093/nar/gkaa176.
7
Highly regulated, diversifying NTP-dependent biological conflict systems with implications for the emergence of multicellularity.高度调控、多样化的 NTP 依赖性生物冲突系统,对多细胞生物的出现具有重要意义。
Elife. 2020 Feb 26;9:e52696. doi: 10.7554/eLife.52696.
8
Structure and mechanism of a Type III CRISPR defence DNA nuclease activated by cyclic oligoadenylate.III 型 CRISPR 防御 DNA 核酸酶的结构与机制:环寡腺苷酸的激活作用
Nat Commun. 2020 Jan 24;11(1):500. doi: 10.1038/s41467-019-14222-x.
9
Cyclic dinucleotides at the forefront of innate immunity.环状二核苷酸处于先天免疫的前沿。
Curr Opin Cell Biol. 2020 Apr;63:49-56. doi: 10.1016/j.ceb.2019.12.004. Epub 2020 Jan 17.
10
An anti-CRISPR viral ring nuclease subverts type III CRISPR immunity.一种抗 CRISPR 病毒环核酶颠覆了 III 型 CRISPR 免疫。
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CARF 结构域超家族的进化和功能分类,原核抗病毒防御的关键传感器。

Evolutionary and functional classification of the CARF domain superfamily, key sensors in prokaryotic antivirus defense.

机构信息

National Center for Biotechnology Information, National Library of Medicine, Bethesda, MD 20894, USA.

Institute of Biotechnology, Life Sciences Center, Vilnius University, Vilnius, Lithuania.

出版信息

Nucleic Acids Res. 2020 Sep 18;48(16):8828-8847. doi: 10.1093/nar/gkaa635.

DOI:10.1093/nar/gkaa635
PMID:32735657
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7498327/
Abstract

CRISPR-associated Rossmann Fold (CARF) and SMODS-associated and fused to various effector domains (SAVED) are key components of cyclic oligonucleotide-based antiphage signaling systems (CBASS) that sense cyclic oligonucleotides and transmit the signal to an effector inducing cell dormancy or death. Most of the CARFs are components of a CBASS built into type III CRISPR-Cas systems, where the CARF domain binds cyclic oligoA (cOA) synthesized by Cas10 polymerase-cyclase and allosterically activates the effector, typically a promiscuous ribonuclease. Additionally, this signaling pathway includes a ring nuclease, often also a CARF domain (either the sensor itself or a specialized enzyme) that cleaves cOA and mitigates dormancy or death induction. We present a comprehensive census of CARF and SAVED domains in bacteria and archaea, and their sequence- and structure-based classification. There are 10 major families of CARF domains and multiple smaller groups that differ in structural features, association with distinct effectors, and presence or absence of the ring nuclease activity. By comparative genome analysis, we predict specific functions of CARF and SAVED domains and partition the CARF domains into those with both sensor and ring nuclease functions, and sensor-only ones. Several families of ring nucleases functionally associated with sensor-only CARF domains are also predicted.

摘要

CRISPR 相关的 Rossmann 折叠(CARF)和 SMODS 相关并融合到各种效应子结构域(SAVED)是基于环状寡核苷酸的抗噬菌体信号系统(CBASS)的关键组成部分,该系统可以感知环状寡核苷酸并将信号传递给诱导细胞休眠或死亡的效应子。大多数 CARF 都是 III 型 CRISPR-Cas 系统中 CBASS 的组成部分,其中 CARF 结构域结合由 Cas10 聚合酶-环化酶合成的环状寡聚 A(cOA),并变构激活效应子,通常是一种混杂的核糖核酸酶。此外,该信号通路还包括一种环核酶,通常也是 CARF 结构域(传感器本身或专门的酶),它可以切割 cOA 并减轻休眠或死亡的诱导。我们展示了细菌和古菌中 CARF 和 SAVED 结构域的全面普查,以及它们基于序列和结构的分类。CARF 结构域有 10 个主要家族和多个较小的群体,它们在结构特征、与不同效应子的关联以及环核酶活性的存在或缺失方面存在差异。通过比较基因组分析,我们预测了 CARF 和 SAVED 结构域的特定功能,并将 CARF 结构域分为具有传感器和环核酶功能的和只有传感器功能的两种。还预测了几种与仅传感器 CARF 结构域功能相关的环核酶家族。