Action of a minimal contractile bactericidal nanomachine

最小收缩杀菌纳米机器的作用

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作者:Peng Ge #, Dean Scholl #, Nikolai S Prokhorov, Jaycob Avaylon, Mikhail M Shneider, Christopher Browning, Sergey A Buth, Michel Plattner, Urmi Chakraborty, Ke Ding, Petr G Leiman, Jeff F Miller, Z Hong Zhou1

Abstract

R-type bacteriocins are minimal contractile nanomachines that hold promise as precision antibiotics1-4. Each bactericidal complex uses a collar to bridge a hollow tube with a contractile sheath loaded in a metastable state by a baseplate scaffold1,2. Fine-tuning of such nucleic acid-free protein machines for precision medicine calls for an atomic description of the entire complex and contraction mechanism, which is not available from baseplate structures of the (DNA-containing) T4 bacteriophage5. Here we report the atomic model of the complete R2 pyocin in its pre-contraction and post-contraction states, each containing 384 subunits of 11 unique atomic models of 10 gene products. Comparison of these structures suggests the following sequence of events during pyocin contraction: tail fibres trigger lateral dissociation of baseplate triplexes; the dissociation then initiates a cascade of events leading to sheath contraction; and this contraction converts chemical energy into mechanical force to drive the iron-tipped tube across the bacterial cell surface, killing the bacterium.

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