The Caspase-1 Digestome Identifies the Glycolysis Pathway as a Target during Infection and Septic Shock

Shao, Wei; Yeretssian, Garabet; Doiron, Karine; Hussain, Sabah N. A.; Saleh, Maya

doi:10.1074/jbc.m708182200

Cited by 286 publications

(269 citation statements)

References 39 publications

(45 reference statements)

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“…We postulate that caspase-1 downstream signaling contributes to the enhanced energy expenditure observed in HFD-fed Casp1 −/− animals. Indeed, using the diagonal gel proteomic approach, several proteins that are involved in energy metabolism were identified as caspase-1 substrates (31). Additional substrates of caspase-1 in adipose tissue may be identified by in silico analysis and may help to explain its contribution to the development of adipose tissue dysfunction during HFD-induced obesity.…”

Section: Discussionmentioning

confidence: 99%

Inflammasome is a central player in the induction of obesity and insulin resistance

Stienstra

Diepen

Tack

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

619

521

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Inflammation plays a key role in the pathogenesis of obesity. Chronic overfeeding leads to macrophage infiltration in the adipose tissue, resulting in proinflammatory cytokine production. Both microbial and endogenous danger signals trigger assembly of the intracellular innate immune sensor Nlrp3, resulting in caspase-1 activation and production of proinflammatory cytokines IL-1β and IL-18. Here, we showed that mice deficient in Nlrp3, apoptosis-associated speck-like protein, and caspase-1 were resistant to the development of high-fat diet-induced obesity, which correlated with protection from obesityinduced insulin resistance. Furthermore, hepatic triglyceride content, adipocyte size, and macrophage infiltration in adipose tissue were all reduced in mice deficient in inflammasome components. Monocyte chemoattractant protein (MCP)-1 is a key molecule that mediates macrophage infiltration. Indeed, defective inflammasome activation was associated with reduced MCP-1 production in adipose tissue. Furthermore, plasma leptin and resistin that affect energy use and insulin sensitivity were also changed by inflammasome-deficiency. Detailed metabolic and molecular phenotyping demonstrated that the inflammasome controls energy expenditure and adipogenic gene expression during chronic overfeeding. These findings reveal a critical function of the inflammasome in obesity and insulin resistance, and suggest inhibition of the inflammasome as a potential therapeutic strategy.

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Section: Discussionmentioning

confidence: 99%

Inflammasome is a central player in the induction of obesity and insulin resistance

Stienstra

Diepen

Tack

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

619

521

View full text Add to dashboard Cite

show abstract

“…Therefore, we propose that processing of substrates by caspase-1 is responsible for the phenotype of pyroptotic cells. 70 Caspase-1 also appears to be required for unconventional protein secretion. 71 The release of cytoplasmic contents is a highly inflammatory event, which underscores the distinct form and function of this programmed cell death.…”

Section: Morphology Of Pyroptotic Cellsmentioning

confidence: 99%

“…99 The elucidation of the caspase-1 digestome identified additional substrates of caspase-1 that are thought to contribute to its effects during the host response to infections and in septic shock. 70 An additional layer of complexity can be attributed to redundancy in pathogeninduced host cell death. Although caspase-1 deficiency renders macrophages resistant to rapid pyroptotic cell death, these cells will nonetheless perish following infection due to the engagement of alternate death pathways.…”

Section: Physiological Significance Of Pyroptosismentioning

confidence: 99%

Cell death in the host response to infection

2008

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“…36 The precise mechanism by which caspase-1 leads to cell death has also been investigated by looking at caspase-1 substrates during infection and inflammation. The caspase-1 digestome includes chaperones, cytoskeletal maintenance components and proteins involved in energy metabolism, 37 as well as caspase-7, 38 which has been shown to be activated downstream of NLRC4 inflammasome during bacterial infection. 39 However, it is still not clear why pyroptotic cells die.…”

Section: Immune Surveillance Systems In Plants and Animalsmentioning

confidence: 99%

Programmed cell death in the plant immune system

2011

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Cell death has a central role in innate immune responses in both plants and animals. Besides sharing striking convergences and similarities in the overall evolutionary organization of their innate immune systems, both plants and animals can respond to infection and pathogen recognition with programmed cell death. The fact that plant and animal pathogens have evolved strategies to subvert specific cell death modalities emphasizes the essential role of cell death during immune responses. The hypersensitive response (HR) cell death in plants displays morphological features, molecular architectures and mechanisms reminiscent of different inflammatory cell death types in animals (pyroptosis and necroptosis). In this review, we describe the molecular pathways leading to cell death during innate immune responses. Additionally, we present recently discovered caspase and caspase-like networks regulating cell death that have revealed fascinating analogies between cell death control across both kingdoms.

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The Caspase-1 Digestome Identifies the Glycolysis Pathway as a Target during Infection and Septic Shock

Cited by 286 publications

References 39 publications

Inflammasome is a central player in the induction of obesity and insulin resistance

Inflammasome is a central player in the induction of obesity and insulin resistance

Cell death in the host response to infection

Programmed cell death in the plant immune system

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