Multiple phage resistance systems inhibit infection via SIR2-dependent NAD+ depletion

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作者
Jeremy Garb
Anna Lopatina
Aude Bernheim
Mindaugas Zaremba
Virginijus Siksnys
Sarah Melamed
Azita Leavitt
Adi Millman
Gil Amitai
Rotem Sorek
机构
[1] Weizmann Institute of Science,Department of Molecular Genetics
[2] Vilnius University,Institute of Biotechnology, Life Sciences Center
[3] University of Vienna,Division of Microbial Ecology, Center for Microbiology and Environmental Systems Science
[4] Université Paris Cité,SEED, U1284, INSERM
来源
Nature Microbiology | 2022年 / 7卷
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摘要
Defence-associated sirtuins (DSRs) comprise a family of proteins that defend bacteria from phage infection via an unknown mechanism. These proteins are common in bacteria and harbour an N-terminal sirtuin (SIR2) domain. In this study we report that DSR proteins degrade nicotinamide adenine dinucleotide (NAD+) during infection, depleting the cell of this essential molecule and aborting phage propagation. Our data show that one of these proteins, DSR2, directly identifies phage tail tube proteins and then becomes an active NADase in Bacillus subtilis. Using a phage mating methodology that promotes genetic exchange between pairs of DSR2-sensitive and DSR2–resistant phages, we further show that some phages express anti-DSR2 proteins that bind and repress DSR2. Finally, we demonstrate that the SIR2 domain serves as an effector NADase in a diverse set of phage defence systems outside the DSR family. Our results establish the general role of SIR2 domains in bacterial immunity against phages.
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页码:1849 / 1856
页数:7
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