Rechkoblit Olga, Sciaky Daniela, Ni Mi, Li Yangmei, Kottur Jithesh, Fang Gang, Aggarwal Aneel K
Department of Pharmacological Sciences, Icahn School of Medicine at Mount Sinai, New York, NY, USA.
Department of Genetics and Genomic Sciences, Icahn School of Medicine at Mount Sinai, New York, NY, USA.
Nat Commun. 2025 Jun 5;16(1):5243. doi: 10.1038/s41467-025-60484-z.
Bacterial CBASS immune defense systems commonly kill virally infected cells by degrading genomic DNA in a form of cell suicide or abortive infection. We present a high-resolution structure of the CBASS effector Cap5, activated by a cyclic nucleotide, in the act of digesting DNA via tetrameric HNH endonuclease domains. Two HNH domains are in a catalytically active state for cleavage of the DNA strands, whereas the other two HNH domains are in a topologically distinct catalytically inactive state for simply DNA binding. The four HNH domains track one face of the DNA and mark an enzyme that acts as a stand-alone non-specific nuclease. We also show that chromosomally encoded CBASS Cap5 can be extrinsically activated by a cyclic nucleotide, as a step towards potential antibiotics.
细菌的CBASS免疫防御系统通常通过以细胞自杀或流产感染的形式降解基因组DNA来杀死病毒感染的细胞。我们展示了由环核苷酸激活的CBASS效应蛋白Cap5在通过四聚体HNH核酸内切酶结构域消化DNA时的高分辨率结构。两个HNH结构域处于催化活性状态以切割DNA链,而另外两个HNH结构域处于拓扑上不同的催化非活性状态,仅用于结合DNA。四个HNH结构域追踪DNA的一个面,并标记一种作为独立非特异性核酸酶起作用的酶。我们还表明,染色体编码的CBASS Cap5可以被环核苷酸外在激活,这是朝着潜在抗生素迈出的一步。
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