Involvement of caspase-4 in IL-1 beta production and pyroptosis in human macrophages during dengue virus infection

Caspase-4 physically interacts with caspase-1 and is believed to be a proinflammatory caspase that can induce the inflammatory form of programmed cell death (pyroptosis) and the release of mature interleukin (IL)-1β. However, the function of caspase-4 in dengue virus infection is not yet fully under...

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Bibliographic Details
Published in:Immunobiology (1979) 2018-04, Vol.223 (4-5), p.356-364
Main Authors: Cheung, Ka Tik, Sze, Daniel Man-yuen, Chan, Kwok Hung, Leung, Polly Hang-mei
Format: Article
Language:English
Subjects:
Caspase 1 - metabolism
Caspase-4
Caspases, Initiator - metabolism
Cells, Cultured
Dengue - immunology
Dengue virus
Dengue Virus - immunology
Humans
Inflammasome
Inflammasomes - metabolism
Interleukin-1beta - metabolism
Interleukin-1β
Macrophages - immunology
Macrophages - virology
Primary Cell Culture
Protein Binding
Pyroptosis
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Summary:Caspase-4 physically interacts with caspase-1 and is believed to be a proinflammatory caspase that can induce the inflammatory form of programmed cell death (pyroptosis) and the release of mature interleukin (IL)-1β. However, the function of caspase-4 in dengue virus infection is not yet fully understood. We examined the function of caspase-4 in IL-1β production and pyroptosis during dengue virus serotype-2 (DENV-2) infection in human macrophages. In this study, DENV-2 infection increased IL-1β protein level with activated caspase-4 activity. Using primary macrophages, we observed that caspase-4 induces activation of caspase-1 and secretion of IL-1β in response to DENV-2 infection, without the need for secondary signals to stimulate the assembly of the inflammasome. These findings indicate that the regulation of caspase-1 activity by capsase-4 could represent a unique mechanism. Our data suggest that caspase-4 is upstream of caspase-1 in the pathway that regulates pyroptosis and IL-1β synthesis in macrophages during DENV-2 infection.
ISSN:0171-2985
1878-3279
DOI:10.1016/j.imbio.2017.10.044