Structural insights into type I and type II Lamassu anti-phage systems
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Bacteria have developed a variety of immune systems to combat phage infections. The Lamassu system is a prokaryotic immune system with a core conserved Structural Maintenance of Chromosomes (SMC) superfamily protein LmuB and diverse effectors named LmuA, whose mechanism remains unclear. Here, we present a series of cryo-electron microscopy structures of type I Lamassu complex from Bacillus cellulasensis and type II Lamassu complex from Vibrio cholerae, both in apo- and dsDNA-bound states, which reveal an unexpected stoichiometry and topological architecture, distinct from canonical SMC complexes. Combined structural and biochemical analyses show how the nuclease effector LmuA is sequestered in an inactive monomeric form within the Lamassu complex, and upon sensing foreign DNA ends, dissociates and assembles into an active tetramer capable of DNA cleavage. Our findings elucidate the mechanism by which Lamassu systems detect viral replication and implement anti-phage defense, highlighting the unprecedented roles of SMC proteins in prokaryotic immunity.