Calcium oxalate crystals induce renal inflammation by NLRP3-mediated IL-1β secretion

Mulay, Shrikant R.; Kulkarni, Onkar P.; Rupanagudi, Khader Valli; Migliorini, Adriana; Darisipudi, Murthy N.; Vilaysane, Akosua; Muruve, Daniel A.; Shi, Yan; Munro, F. L.; Liapis, Helen; Anders, Hans‐Joachim

doi:10.1172/jci63679

Cited by 400 publications

(383 citation statements)

References 49 publications

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“…The cytosolic innate immune receptor Nlrp3 is able to sense cellular damage 13 and mediates renal inflammation and pathological characteristics after IR 14e16 or nephrocalcinosis. 17 Next to the detrimental role of Nlrp3 in different renal disease models and consistent with the dual role of TLR2, Nlrp3 was shown to protect against loss of colonic epithelial integrity. 18 We, therefore, speculate that Nlrp3, which contributes to sterile renal inflammation during acute renal IR injury, might also drive subsequent tubular repair.…”

mentioning

confidence: 76%

A Tissue-Specific Role for Nlrp3 in Tubular Epithelial Repair after Renal Ischemia/Reperfusion

Bakker

Butter

Claessen

et al. 2014

The American Journal of Pathology

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mentioning

confidence: 76%

A Tissue-Specific Role for Nlrp3 in Tubular Epithelial Repair after Renal Ischemia/Reperfusion

Bakker

Butter

Claessen

et al. 2014

The American Journal of Pathology

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“…Our data suggest that cystine crystals may not be inert but rather a trigger of inflammation, as recently demonstrated for calcium oxalate crystals in nephrocalcinosis. 17 Elevated circulating levels of IL-1b and IL-18 in cystinotic patients and elevated inflammasome-related gene expression both in PBMCs from patients and in kidney tissue from Ctns 2/2 mice support the hy pothesis that inflammasome activation may contribute to the development of the interstitial inflammation and fibrosis leading to ESRD observed in cystinotic patients and mice. Interestingly, the inflammasome-regulated cytokines IL-1b and IL-18 are implicated in several animal models or human forms of CKD.…”

mentioning

confidence: 82%

Inflammasome Activation by Cystine Crystals

Prencipe

Caiello

Cherqui

et al. 2014

Journal of the American Society of Nephrology

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Intralysosomal cystine crystal accumulation, due to mutations in the CTNS gene, is a hallmark of nephropathic cystinosis, but the role of these crystals in disease pathogenesis remains unclear. We hypothesized that, similar to other host-derived crystalline moieties, cystine crystals can induce IL-1b production through inflammasome activation. Thus, we investigated the proinflammatory effects of cystine crystals in primary human PBMCs. LPS-primed PBMCs stimulated with cystine crystals secreted IL-1b in a dose-dependent manner. Similarly to IL-1b secretion induced by other crystalline inflammasome activators, cystine crystal-induced IL-1b secretion required activation of caspase-1. Additionally, exogenous cystine crystals were internalized by monocytes, and inhibition of phagocytosis, cathepsin B leakage, generation of reactive oxygen species, and potassium efflux reduced cystine crystalinduced IL-1b secretion. Patients with cystinosis had higher levels of circulating IL-1b and IL-18 compared with controls. Analysis of inflammasome-related gene expression in PBMCs from patients with cystinosis revealed a significant increase in IL-1b and CASP-1 transcript levels compared with controls. Moreover, knockout of cystinosin in mice led to significant increases in serum IL-18 levels and kidney expression of inflammasome-related genes Pycard, Il18r1, Il1r1, and Il1rl2). Taken together, these data demonstrate that cystine crystals are endogenous inflammasome-activating stimuli, suggesting a novel role for cystine crystals in the pathogenesis of nephropathic cystinosis.

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“…Having identified ferroptosis to be of relevance in acute postischemic injury, we sought to investigate another model of acute renal failure, oxalate nephropathy, which has recently been established (30). Intrarenal CaOx crystal deposition was identical in all groups ( Fig.…”

Section: Ferroptosis Mediates Tubule Necrosis In Oxalate Nephropathymentioning

confidence: 99%

Synchronized renal tubular cell death involves ferroptosis

Linkermann

Skouta

Himmerkus

et al. 2014

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

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869

804

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Receptor-interacting protein kinase 3 (RIPK3)-mediated necroptosis is thought to be the pathophysiologically predominant pathway that leads to regulated necrosis of parenchymal cells in ischemia-reperfusion injury (IRI), and loss of either Fas-associated protein with death domain (FADD) or caspase-8 is known to sensitize tissues to undergo spontaneous necroptosis. Here, we demonstrate that renal tubules do not undergo sensitization to necroptosis upon genetic ablation of either FADD or caspase-8 and that the RIPK1 inhibitor necrostatin-1 (Nec-1) does not protect freshly isolated tubules from hypoxic injury. In contrast, irondependent ferroptosis directly causes synchronized necrosis of renal tubules, as demonstrated by intravital microscopy in models of IRI and oxalate crystal-induced acute kidney injury. To suppress ferroptosis in vivo, we generated a novel third-generation ferrostatin (termed 16-86), which we demonstrate to be more stable, to metabolism and plasma, and more potent, compared with the firstin-class compound ferrostatin-1 (Fer-1). Even in conditions with extraordinarily severe IRI, 16-86 exerts strong protection to an extent which has not previously allowed survival in any murine setting. In addition, 16-86 further potentiates the strong protective effect on IRI mediated by combination therapy with necrostatins and compounds that inhibit mitochondrial permeability transition. Renal tubules thus represent a tissue that is not sensitized to necroptosis by loss of FADD or caspase-8. Finally, ferroptosis mediates postischemic and toxic renal necrosis, which may be therapeutically targeted by ferrostatins and by combination therapy.

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Calcium oxalate crystals induce renal inflammation by NLRP3-mediated IL-1β secretion

Cited by 400 publications

References 49 publications

A Tissue-Specific Role for Nlrp3 in Tubular Epithelial Repair after Renal Ischemia/Reperfusion

A Tissue-Specific Role for Nlrp3 in Tubular Epithelial Repair after Renal Ischemia/Reperfusion

Inflammasome Activation by Cystine Crystals

Synchronized renal tubular cell death involves ferroptosis

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