[HTML][HTML] Innate immune sensing of bacterial modifications of Rho GTPases by the Pyrin inflammasome

H Xu, J Yang, W Gao, L Li, P Li, L Zhang, YN Gong… - Nature, 2014 - nature.com
H Xu, J Yang, W Gao, L Li, P Li, L Zhang, YN Gong, X Peng, JJ Xi, S Chen, F Wang, F Shao
Nature, 2014nature.com
Cytosolic inflammasome complexes mediated by a pattern recognition receptor (PRR)
defend against pathogen infection by activating caspase 1. Pyrin, a candidate PRR, can
bind to the inflammasome adaptor ASC to form a caspase 1-activating complex,. Mutations
in the Pyrin-encoding gene, MEFV, cause a human autoinflammatory disease known as
familial Mediterranean fever,,. Despite important roles in immunity and disease, the
physiological function of Pyrin remains unknown. Here we show that Pyrin mediates …
Abstract
Cytosolic inflammasome complexes mediated by a pattern recognition receptor (PRR) defend against pathogen infection by activating caspase 1. Pyrin, a candidate PRR, can bind to the inflammasome adaptor ASC to form a caspase 1-activating complex,. Mutations in the Pyrin-encoding gene, MEFV, cause a human autoinflammatory disease known as familial Mediterranean fever,,. Despite important roles in immunity and disease, the physiological function of Pyrin remains unknown. Here we show that Pyrin mediates caspase 1 inflammasome activation in response to Rho-glucosylation activity of cytotoxin TcdB,,, a major virulence factor of Clostridium difficile, which causes most cases of nosocomial diarrhoea. The glucosyltransferase-inactive TcdB mutant loses the inflammasome-stimulating activity. Other Rho-inactivating toxins, including FIC-domain adenylyltransferases (Vibrio parahaemolyticus VopS and Histophilus somni IbpA) and Clostridium botulinum ADP-ribosylating C3 toxin, can also biochemically activate the Pyrin inflammasome in their enzymatic activity-dependent manner. These toxins all target the Rho subfamily and modify a switch-I residue. We further demonstrate that Burkholderia cenocepacia inactivates RHOA by deamidating Asn 41, also in the switch-I region, and thereby triggers Pyrin inflammasome activation, both of which require the bacterial type VI secretion system (T6SS). Loss of the Pyrin inflammasome causes elevated intra-macrophage growth of B. cenocepacia and diminished lung inflammation in mice. Thus, Pyrin functions to sense pathogen modification and inactivation of Rho GTPases, representing a new paradigm in mammalian innate immunity.
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