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Inhibition of inflammasome activation by Coxiella burnetii type IV secretion system effector IcaA.


ABSTRACT: Coxiella burnetii is a highly infectious bacterium that promotes its own replication in macrophages by inhibiting several host cell responses. Here, we show that C. burnetii inhibits caspase-1 activation in primary mouse macrophages. By using co-infection experiments, we determine that the infection of macrophages with C. burnetii inhibits the caspase-11-mediated non-canonical activation of the NLRP3 inflammasome induced by subsequent infection with Escherichia coli or Legionella pneumophila. Genetic screening using flagellin mutants of L. pneumophila as a surrogate host, reveals a novel C. burnetii gene (IcaA) involved in the inhibition of caspase activation. Expression of IcaA in L. pneumophila inhibited the caspase-11 activation in macrophages. Moreover, icaA(-) mutants of C. burnetii failed to suppress the caspase-11-mediated inflammasome activation induced by L. pneumophila. Our data reveal IcaA as a novel C. burnetii effector protein that is secreted by the Dot/Icm type IV secretion system and interferes with the caspase-11-induced, non-canonical activation of the inflammasome.

SUBMITTER: Cunha LD 

PROVIDER: S-EPMC4703858 | biostudies-other | 2015 Dec

REPOSITORIES: biostudies-other

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Inhibition of inflammasome activation by Coxiella burnetii type IV secretion system effector IcaA.

Cunha Larissa D LD   Ribeiro Juliana M JM   Fernandes Talita D TD   Massis Liliana M LM   Khoo Chen Ai CA   Moffatt Jennifer H JH   Newton Hayley J HJ   Roy Craig R CR   Zamboni Dario S DS  

Nature communications 20151221


Coxiella burnetii is a highly infectious bacterium that promotes its own replication in macrophages by inhibiting several host cell responses. Here, we show that C. burnetii inhibits caspase-1 activation in primary mouse macrophages. By using co-infection experiments, we determine that the infection of macrophages with C. burnetii inhibits the caspase-11-mediated non-canonical activation of the NLRP3 inflammasome induced by subsequent infection with Escherichia coli or Legionella pneumophila. Ge  ...[more]

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