Structural basis for broad anti-phage immunity by DISARM

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作者
Jack P. K. Bravo
Cristian Aparicio-Maldonado
Franklin L. Nobrega
Stan J. J. Brouns
David W. Taylor
机构
[1] University of Texas at Austin,Department of Molecular Biosciences
[2] Delft University of Technology,Department of Bionanoscience
[3] Kavli Institute of Nanoscience,School of Biological Sciences
[4] University of Southampton,Interdisciplinary Life Sciences Graduate Programs
[5] University of Texas at Austin,Center for Systems and Synthetic Biology
[6] University of Texas at Austin,LIVESTRONG Cancer Institutes
[7] Dell Medical School,undefined
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In the evolutionary arms race against phage, bacteria have assembled a diverse arsenal of antiviral immune strategies. While the recently discovered DISARM (Defense Island System Associated with Restriction-Modification) systems can provide protection against a wide range of phage, the molecular mechanisms that underpin broad antiviral targeting but avoiding autoimmunity remain enigmatic. Here, we report cryo-EM structures of the core DISARM complex, DrmAB, both alone and in complex with an unmethylated phage DNA mimetic. These structures reveal that DrmAB core complex is autoinhibited by a trigger loop (TL) within DrmA and binding to DNA substrates containing a 5′ overhang dislodges the TL, initiating a long-range structural rearrangement for DrmAB activation. Together with structure-guided in vivo studies, our work provides insights into the mechanism of phage DNA recognition and specific activation of this widespread antiviral defense system.
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