Structural insights into activation mechanisms on NADase of the bacterial DSR2 anti-phage defense system
文献类型: 外文期刊
第一作者: Zhang, Hong
作者: Zhang, Hong;Li, Lanlan;Chen, Lifei;Sun, Lifang;Dong, Panpan;Jing, Dingding;Yang, Jinbo;Fu, Lei;Xiao, Fangnan;Wu, Yunkun;Zhang, Hong;Li, Lanlan;Chen, Lifei;Sun, Lifang;Dong, Panpan;Jing, Dingding;Yang, Jinbo;Fu, Lei;Xiao, Fangnan;Wu, Yunkun;Li, Yu;Xia, Ningshao;Li, Shaowei;Zheng, Qingbing;Li, Yu;Xia, Ningshao;Li, Shaowei;Zheng, Qingbing;Zhu, Chunhua
作者机构:
期刊名称:SCIENCE ADVANCES ( 影响因子:11.7; 五年影响因子:13.7 )
ISSN: 2375-2548
年卷期: 2024 年 10 卷 31 期
页码:
收录情况: SCI
摘要: As a sirtuin (SIR2) family protein, defense-associated sirtuin2 (DSR2) has been demonstrated to participate in bacterial anti-phage resistance via depleting nicotinamide adenine dinucleotide (NAD+) of infected cells, which can be activated by tail tube protein (TTP) and inhibited by DSR anti-defense 1 (DSAD1) of diverse phages. However, the regulating mechanism remains elusive. Here, we determined the cryo-electron microscopy structure of apo DSR2, as well as the respective complex structures with TTP and DSAD1. Structural analyses and biochemical studies reveal that DSR2 forms a tetramer with a SIR2 central core and two distinct conformations. Monomeric TTP preferentially binds to the closed conformation of DSR2, inducing conformational distortions on SIR2 tetramer assembly to activate its NADase activity. DSAD1 combines with the open conformation of DSR2, directly or allosterically inhibiting TTP activation on DSR2 NAD+ hydrolysis. Our findings decipher the detailed molecule mechanisms for DSR2 NADase activity regulation and lay a foundation for in-depth understanding of the DSR2 anti-phage defense system.
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