Envelope stress responses defend against type six secretion system attacks independently of immunity proteins
The arms race among microorganisms is a key driver in the evolution of not only the weapons but also defence mechanisms. Many Gram-negative bacteria use the type six secretion system (T6SS) to deliver toxic effectors directly into neighbouring cells. Defence against effectors requires cognate immuni...
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Veröffentlicht in: | Nature microbiology 2020-05, Vol.5 (5), p.706-714 |
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Sprache: | eng |
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Zusammenfassung: | The arms race among microorganisms is a key driver in the evolution of not only the weapons but also defence mechanisms. Many Gram-negative bacteria use the type six secretion system (T6SS) to deliver toxic effectors directly into neighbouring cells. Defence against effectors requires cognate immunity proteins. However, here we show immunity-independent protection mediated by envelope stress responses in
Escherichia coli
and
Vibrio cholerae
against a
V. cholerae
T6SS effector, TseH. We demonstrate that TseH is a PAAR-dependent species-specific effector highly potent against
Aeromonas
species but not against its
V. cholerae
immunity mutant or
E. coli
. A structural analysis reveals TseH is probably a NlpC/P60-family cysteine endopeptidase. We determine that two envelope stress-response pathways, Rcs and BaeSR, protect
E. coli
from TseH toxicity by mechanisms including capsule synthesis. The two-component system WigKR (VxrAB) is critical for protecting
V. cholerae
from its own T6SS despite expressing immunity genes. WigR also regulates T6SS expression, suggesting a dual role in attack and defence. This deepens our understanding of how bacteria survive T6SS attacks and suggests that defence against the T6SS represents a major selective pressure driving the evolution of species-specific effectors and protective mechanisms mediated by envelope stress responses and capsule synthesis.
Defence against type six secretion system (T6SS) effectors is thought to be mostly mediated by dedicated immunity proteins that antagonize specific effector proteins. Here, two envelope stress-response pathways, Rcs and BaeSR, are shown to regulate protection against the T6SS effector TseH by modulating the integrity of the bacterial envelope in a manner independent of immunity proteins. |
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ISSN: | 2058-5276 2058-5276 |
DOI: | 10.1038/s41564-020-0672-6 |