Activation of the IL-1β-Processing Inflammasome Is Involved in Contact Hypersensitivity

Watanabe, Hideki; Gaide, Olivier; Pétrilli, Virginie; Martinon, Fabio; Contassot, Emmanuel; Roques, Stéphanie; Kummer, J. Alain; Tschopp, Jürg; French, Lars E.

doi:10.1038/sj.jid.5700819

Cited by 362 publications

(349 citation statements)

References 42 publications

(59 reference statements)

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“…The principle function of the inflammasome is the cleavage, by the protease, caspase-1, of precursor interleukin molecules into the forms, IL-1b and IL-18 and the subsequent release of these proinflammatory cytokines into the extracellular space (Watanabe et al, 2007). This process involves three steps: firstly, synthesis of precursor molecules, e.g.…”

Section: The Role Of P2x Receptors In Neuroinflammationmentioning

confidence: 99%

Purinergic mechanisms in neuroinflammation: An update from molecules to behavior

et al. 2016

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a b s t r a c tThe principle functions of neuroinflammation are to limit tissue damage and promote tissue repair in response to pathogens or injury. While neuroinflammation has utility, pathophysiological inflammatory responses, to some extent, underlie almost all neuropathology. Understanding the mechanisms that control the three stages of inflammation (initiation, propagation and resolution) is therefore of critical importance for developing treatments for diseases of the central nervous system. The purinergic signaling system, involving adenosine, ATP and other purines, plus a host of P1 and P2 receptor subtypes, controls inflammatory responses in complex ways. Activation of the inflammasome, leading to release of pro-inflammatory cytokines, activation and migration of microglia and altered astroglial function are key regulators of the neuroinflammatory response. Here, we review the role of P1 and P2 receptors in mediating these processes and examine their contribution to disorders of the nervous system. Firstly, we give an overview of the concept of neuroinflammation. We then discuss the contribution of P2X, P2Y and P1 receptors to the underlying processes, including a discussion of cross-talk between these different pathways. Finally, we give an overview of the current understanding of purinergic contributions to neuroinflammation in the context of specific disorders of the central nervous system, with special emphasis on neuropsychiatric disorders, characterized by chronic low grade inflammation or maternal inflammation. An understanding of the important purinergic contribution to neuroinflammation underlying neuropathology is likely to be a necessary step towards the development of effective interventions.

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Section: The Role Of P2x Receptors In Neuroinflammationmentioning

confidence: 99%

Purinergic mechanisms in neuroinflammation: An update from molecules to behavior

et al. 2016

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“…We have recently reported that Hcys can activate NALP3 inflammasomes in podocytes, an intracellular molecular switch of inflammation (33). Inflammasome activation has also been implicated in a number of inflammatory and metabolic diseases, including obesity, gout, hypersensitivity, silicosis, and diabetes, where inhibition of the inflammasome proteins NALP3, ASC, or caspase-1 significantly attenuates the downstream inflammatory reaction produced under these conditions (3,17,26,36). Similarly, our report showed that inhibition of either ASC or caspase-1 could prevent podocyte and glomerular damage induced by hHcys, improving renal structural and functional integrity (33), suggesting an important role for inflammasome activation in mediating the deleterious effects of hHcys.…”

Section: Nadph Oxidase and Inflammasome Activation In Podocytesmentioning

confidence: 99%

NADPH Oxidase-Mediated Triggering of Inflammasome Activation in Mouse Podocytes and Glomeruli During Hyperhomocysteinemia

Abais

Zhang

Xia

et al. 2013

Antioxidants & Redox Signaling

127

133

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Aim: Our previous studies have shown that NOD-like receptor protein (NALP3) inflammasome activation is importantly involved in podocyte dysfunction and glomerular sclerosis induced by hyperhomocysteinemia (hHcys). The present study was designed to test whether nicotinamide adenine dinucleotide phosphate (NADPH) oxidase-mediated redox signaling contributes to homocysteine (Hcys)-induced activation of NALP3 inflammasomes, an intracellular inflammatory machinery in podocytes in vitro and in vivo. Results: In vitro confocal microscopy and size-exclusion chromatography revealed that upon NADPH oxidase inhibition by gp91 phox siRNA, gp91ds-tat peptide, diphenyleneiodonium, or apocynin, aggregation of inflammasome proteins NALP3, apoptosis-associated speck-like protein (ASC), and caspase-1 was significantly attenuated in mouse podocytes. This NADPH oxidase inhibition also resulted in diminished Hcys-induced inflammasome activation, evidenced by reduced caspase-1 activity and interleukin-1b production. Similar findings were observed in vivo where gp91phox -/ -mice and mice receiving a gp91ds-tat treatment exhibited markedly reduced inflammasome formation and activation. Further, in vivo NADPH oxidase inhibition protected the glomeruli and podocytes from hHcys-induced injury as shown by attenuated proteinuria, albuminuria, and glomerular sclerotic changes. This might be attributed to the fact that gp91phox -/ -and gp91ds-tat-treated mice had abolished infiltration of macrophages and T-cells into the glomeruli during hHcys. Innovation: Our study for the first time links NADPH oxidase to the formation and activation of NALP3 inflammasomes in podocytes. Conclusion: Hcys-induced NADPH oxidase activation is importantly involved in the switching on of NALP3 inflammasomes within podocytes, which leads to the downstream recruitment of immune cells, ultimately resulting in glomerular injury and sclerosis. Antioxid. Redox Signal. 18, 1537-1548.

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“…[18][19][20] Furthermore, 'danger-associated molecular patterns or DAMPs' (non-microbial/pathogenic) such as ATP, imidazoquinoline, monosodium urate crystals (MSU) and the skin irritant trinitrochlorobenzene have been shown to induce NALP3 inflammasome activity. 16,19,[21][22][23] Similar to NALP3, the NALP1 inflammasome can be activated by MDP. 5,15 Moreover, in mice activation of caspase-1 by lethal toxin of B. anthracis is dependent on a functional NALP1b.…”

mentioning

confidence: 99%

Activation of the NALP3 inflammasome is triggered by low intracellular potassium concentration

et al. 2007

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Activation of the IL-1β-Processing Inflammasome Is Involved in Contact Hypersensitivity

Cited by 362 publications

References 42 publications

Purinergic mechanisms in neuroinflammation: An update from molecules to behavior

Purinergic mechanisms in neuroinflammation: An update from molecules to behavior

NADPH Oxidase-Mediated Triggering of Inflammasome Activation in Mouse Podocytes and Glomeruli During Hyperhomocysteinemia

Activation of the NALP3 inflammasome is triggered by low intracellular potassium concentration

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