AI Article Synopsis
- * Caspase-11 is a specific inflammatory caspase that gets activated by bacterial LPS, leading to its aggregation and the cleavage of gasdermin D, which causes a form of cell death known as pyroptosis.
- * Research found that the activation and self-processing of Caspase-11 are essential for its assembly into speckles in macrophages in response to LPS, indicating a crucial role for its enzymatic activity in inflammasome organization.
Article Abstract
Inflammatory caspases are cysteine protease zymogens whose activation following infection or cellular damage occurs within supramolecular organizing centers (SMOCs) known as inflammasomes. Inflammasomes recruit caspases to undergo proximity-induced autoprocessing into an enzymatically active form that cleaves downstream targets. Binding of bacterial LPS to its cytosolic sensor, caspase-11 (Casp11), promotes Casp11 aggregation within a high-molecular-weight complex known as the noncanonical inflammasome, where it is activated to cleave gasdermin D and induce pyroptosis. However, the cellular correlates of Casp11 oligomerization and whether Casp11 forms an LPS-induced SMOC within cells remain unknown. Expression of fluorescently labeled Casp11 in macrophages revealed that cytosolic LPS induced Casp11 speck formation. Unexpectedly, catalytic activity and autoprocessing were required for Casp11 to form LPS-induced specks in macrophages. Furthermore, both catalytic activity and autoprocessing were required for Casp11 speck formation in an ectopic expression system, and processing of Casp11 via ectopically expressed TEV protease was sufficient to induce Casp11 speck formation. These data reveal a previously undescribed role for Casp11 catalytic activity and autoprocessing in noncanonical inflammasome assembly, and shed new light on the molecular requirements for noncanonical inflammasome assembly in response to cytosolic LPS.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10794067 | PMC |
| http://dx.doi.org/10.7554/eLife.83725 | DOI Listing |
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