Departamento de Genética y Microbiología, Área de Genética (Unidad Asociada al IQF-CSIC), Universidad de Murcia, 30100 Murcia, Spain.
Instituto de Química Física "Blas Cabrera," CSIC (IQF-CSIC), 28006 Madrid, Spain.
Sci Adv. 2024 Oct 25;10(43):eadp1053. doi: 10.1126/sciadv.adp1053.
How CRISPR-Cas and cyclic oligonucleotide-based antiphage signaling systems (CBASS) are coordinately deployed against invaders remains unclear. We show that a locus containing two CBASS and one type III-B CRISPR-Cas system, regulated by the transmembrane anti-σ DdvA and its cognate extracytoplasmic function (ECF) σ DdvS, can defend against a phage. Cryo-electron microscopy reveals DdvA-DdvS pairs assemble as arrow-shaped transmembrane dimers. Each DdvA periplasmic domain adopts a separase/craspase-type tetratricopeptide repeat (TPR)-caspase HetF-associated with TPR (TPR-CHAT) architecture with an incomplete His-Cys active site, lacking three α-helices conserved among CHAT domains. Each active site faces the dimer interface, raising the possibility that signal-induced caspase-like DdvA autoproteolysis in trans precedes RseP-mediated intramembrane proteolysis and DdvS release. Nuclear magnetic resonance reveals a DdvA cytoplasmic CHCC-type zinc-bound three-helix bundle that binds to DdvS σ and σ domains, undergoing σ-induced helix extension to trap DdvS. Altogether, we provide structural-mechanistic insights into membrane anti-σ-ECF σ regulation of an antiviral CBASS-CRISPR-Cas defense island.
CRISPR-Cas 和基于环状寡核苷酸的抗噬菌体信号系统(CBASS)如何协同部署以抵御入侵者尚不清楚。我们表明,一个包含两个 CBASS 和一个 III-B 型 CRISPR-Cas 系统的基因座,由跨膜抗σ DdvA 及其同源胞外功能(ECF)σ DdvS 调控,可以抵御噬菌体。冷冻电子显微镜揭示了 DdvA-DdvS 对组装成箭头状的跨膜二聚体。每个 DdvA 周质域采用分离酶/半胱天冬酶型四肽重复(TPR)-与 TPR(TPR-CHAT)结构相关的半胱天冬酶 HetF,具有不完整的 His-Cys 活性位点,缺乏 CHAT 结构域中保守的三个α-螺旋。每个活性位点都面向二聚体界面,这增加了信号诱导的 DdvA 自身切割的可能性,这种切割发生在 RseP 介导的跨膜蛋白酶解和 DdvS 释放之前。核磁共振揭示了 DdvA 细胞质 CHCC 型锌结合的三螺旋束,该结构与 DdvS σ 和 σ 结构域结合,经历 σ 诱导的螺旋延伸以捕获 DdvS。总的来说,我们提供了对膜抗σ-ECF σ 调控抗病毒 CBASS-CRISPR-Cas 防御岛的结构-机制见解。
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