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Rsm(Csr)转录后调控途径协调控制多个 CRISPR-Cas 免疫系统。

The Rsm (Csr) post-transcriptional regulatory pathway coordinately controls multiple CRISPR-Cas immune systems.

机构信息

Department of Microbiology and Immunology, University of Otago, PO Box 56, Dunedin 9054, New Zealand.

Bio-Protection Research Centre, University of Otago, PO Box 56, Dunedin 9054, New Zealand.

出版信息

Nucleic Acids Res. 2021 Sep 20;49(16):9508-9525. doi: 10.1093/nar/gkab704.

Abstract

CRISPR-Cas systems provide bacteria with adaptive immunity against phages and plasmids; however, pathways regulating their activity are not well defined. We recently developed a high-throughput genome-wide method (SorTn-seq) and used this to uncover CRISPR-Cas regulators. Here, we demonstrate that the widespread Rsm/Csr pathway regulates the expression of multiple CRISPR-Cas systems in Serratia (type I-E, I-F and III-A). The main pathway component, RsmA (CsrA), is an RNA-binding post-transcriptional regulator of carbon utilisation, virulence and motility. RsmA binds cas mRNAs and suppresses type I and III CRISPR-Cas interference in addition to adaptation by type I systems. Coregulation of CRISPR-Cas and flagella by the Rsm pathway allows modulation of adaptive immunity when changes in receptor availability would alter susceptibility to flagella-tropic phages. Furthermore, we show that Rsm controls CRISPR-Cas in other genera, suggesting conservation of this regulatory strategy. Finally, we identify genes encoding RsmA homologues in phages, which have the potential to manipulate the physiology of host bacteria and might provide an anti-CRISPR activity.

摘要

CRISPR-Cas 系统为细菌提供了针对噬菌体和质粒的适应性免疫;然而,调节其活性的途径尚未得到很好的定义。我们最近开发了一种高通量的全基因组方法(SorTn-seq),并利用该方法发现了 CRISPR-Cas 的调控因子。在这里,我们证明了广泛存在的 Rsm/Csr 途径调节了沙雷氏菌(I-E、I-F 和 III-A 型)中多个 CRISPR-Cas 系统的表达。主要途径成分 RsmA(CsrA)是一种 RNA 结合的碳利用、毒力和运动性的转录后调控因子。RsmA 结合 cas mRNA,并抑制 I 型和 III 型 CRISPR-Cas 的干扰,除了 I 型系统的适应外。Rsm 途径对 CRISPR-Cas 和鞭毛的共同调控允许在受体可用性发生变化时调节适应性免疫,从而改变对鞭毛噬菌体的易感性。此外,我们还表明 Rsm 控制其他属中的 CRISPR-Cas,表明这种调控策略具有保守性。最后,我们在噬菌体中鉴定出编码 RsmA 同源物的基因,这些基因有可能操纵宿主细菌的生理学,并可能具有抗 CRISPR 活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec7a/8450108/64f223c4547e/gkab704fig1.jpg

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