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Merck

Shigella evades pyroptosis by arginine ADP-riboxanation of caspase-11.

Nature (2021-10-22)
Zilin Li, Wang Liu, Jiaqi Fu, Sen Cheng, Yue Xu, Zhiqiang Wang, Xiaofan Liu, Xuyan Shi, Yaxin Liu, Xiangbing Qi, Xiaoyun Liu, Jingjin Ding, Feng Shao
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Mouse caspase-11 and human caspase-4ย and caspase-5 recognize cytosolic lipopolysaccharide (LPS) to induce pyroptosis by cleaving the pore-forming protein GSDMD1-5. This non-canonical inflammasome defends against Gram-negative bacteria6,7. Shigella flexneri, which causes bacillary dysentery, lives freely within theย host cytosol where these caspases reside. However, the role of caspase-11-mediated pyroptosis in S.โ€‰flexneri infection is unknown. Here we show that caspase-11 did not protect mice from S.โ€‰flexneri infection, in contrast to infection with another cytosolic bacterium, Burkholderia thailandensis8. S.โ€‰flexneri evaded pyroptosis mediated byย caspase-11ย or caspaseย 4ย (hereafter referred to as caspase-11/4) using a type III secretion system (T3SS)ย effector, OspC3. OspC3, but not its paralogues OspC1ย andย 2, covalently modified caspase-11/4; although it used the NAD+ donor, this modificationย was not ADP-ribosylation. Biochemical dissections uncovered an ADP-riboxanation modification on Arg314ย and Arg310 in caspase-4ย and caspase-11, respectively. The enzymatic activity was shared by OspC1ย andย 2, whose ankyrin-repeat domains, unlike that of OspC3, could not recognize caspase-11/4. ADP-riboxanation of the arginine blocked autoprocessing ofย caspase-4/11 as well as their recognition and cleavage of GSDMD. ADP-riboxanation ofย caspase-11 paralysed pyroptosis-mediated defence in Shigella-infected miceย and mutation of ospC3 stimulated caspase-11- andย GSDMD-dependent anti-Shigella humoral immunity, generating a vaccine-like protective effect. Our study establishes ADP-riboxanation of arginine as a bacterial virulence mechanism that prevents LPS-induced pyroptosis.

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