Structural and mechanistic basis of immunity toward endonuclease colicins

被引:0
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作者
Colin Kleanthous
Ulrike C. Kühlmann
Ansgar J. Pommer
Neil Ferguson
Sheena E. Radford
Geoffrey R. Moore
Richard James
Andrew M. Hemmings
机构
[1] School of Biological Sciences,
[2] University of East Anglia,undefined
[3] School of Biochemistry and Molecular Biology,undefined
[4] University of Leeds,undefined
[5] School of Chemical Sciences,undefined
[6] University of East Anglia,undefined
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摘要
The crystal structure of the cytotoxic endonuclease domain from the bacterial toxin colicin E9 in complex with its cognate immunity protein Im9 reveals that the inhibitor does not bind at the active site, the core of which comprises the HNH motif found in intron-encoded homing endonucleases, but rather at an adjacent position leaving the active site exposed yet unable to bind DNA because of steric and electrostatic clashes with incoming substrate. Although its mode of action is unorthodox, Im9 is a remarkably effective inhibitor since it folds within milliseconds and then associates with its target endonuclease at the rate of diffusion to form an inactive complex with sub-femtomolar binding affinity. This hyperefficient mechanism of inhibition could be well suited to other toxic enzyme systems, particularly where the substrate is a polymer extending beyond the boundaries of the active site.
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页码:243 / 252
页数:9
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