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Structure of a peptidoglycan amidase effector targeted to Gram-negative bacteria by the type VI secretion system.


ABSTRACT: The target range of a bacterial secretion system can be defined by effector substrate specificity or by the efficacy of effector delivery. Here, we report the crystal structure of Tse1, a type VI secretion (T6S) bacteriolytic amidase effector from Pseudomonas aeruginosa. Consistent with its role as a toxin, Tse1 has a more accessible active site than related housekeeping enzymes. The activity of Tse1 against isolated peptidoglycan shows its capacity to act broadly against Gram-negative bacteria and even certain Gram-positive species. Studies with intact cells indicate that Gram-positive bacteria can remain vulnerable to Tse1 despite cell wall modifications. However, interbacterial competition studies demonstrate that Tse1-dependent lysis is restricted to Gram-negative targets. We propose that the previously observed specificity for T6S against Gram-negative bacteria is a consequence of high local effector concentration achieved by T6S-dependent targeting to its site of action rather than inherent effector substrate specificity.

SUBMITTER: Chou S 

PROVIDER: S-EPMC3401384 | biostudies-literature | 2012 Jun

REPOSITORIES: biostudies-literature

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Structure of a peptidoglycan amidase effector targeted to Gram-negative bacteria by the type VI secretion system.

Chou Seemay S   Bui Nhat Khai NK   Russell Alistair B AB   Lexa Katrina W KW   Gardiner Taylor E TE   LeRoux Michele M   Vollmer Waldemar W   Mougous Joseph D JD  

Cell reports 20120531 6


The target range of a bacterial secretion system can be defined by effector substrate specificity or by the efficacy of effector delivery. Here, we report the crystal structure of Tse1, a type VI secretion (T6S) bacteriolytic amidase effector from Pseudomonas aeruginosa. Consistent with its role as a toxin, Tse1 has a more accessible active site than related housekeeping enzymes. The activity of Tse1 against isolated peptidoglycan shows its capacity to act broadly against Gram-negative bacteria  ...[more]

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