Tyrosine kinase inhibitors trigger lysosomal damage-associated cell lysis to activate the NLRP3 inflammasome

Neuwirt, Emilia; Magnani, Giovanni; Ćiković, Tamara; Костина, Анна Владимировна; Wöhrle, Svenja; Flemming, Stephan; Fischenich, Nora J.; Saller, Benedikt S.; Gorka, Oliver; Renner, Steffen; Agarinis, Claudia; Parker, Christian N.; Boettcher, Andreas; Farady, Christopher J.; Backofen, Rolf; Rodriguez‐Franco, Marta; Tholen, Martina; Reinheckel, Thomas; Ott, Thomas; Groß, Christina; Jost, Philipp J.; Groß, Olaf

doi:10.1101/2022.02.19.480941

Cited by 2 publications

(1 citation statement)

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“…Other tyrosine kinase inhibitors, including dasatinib and ponatinib, have demonstrated a reduction in lung inflammation and fibrosis in mouse silicosis models [64,65]. However, somewhat conflictingly, tyrosine kinase inhibitors may activate the NLRP3 inflammasome, as demonstrated in in-vitro studies of myeloid cells [66] (Table 3). This suggests further research is required in this area.…”

Section: Antifibrotic Therapymentioning

confidence: 99%

Toward targeted treatments for silicosis

Barnes,

Lam,

Tate

et al. 2023

Current Opinion in Pulmonary Medicine

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Purpose of review There has been a rapid increase in silicosis cases, particularly related to artificial stone. The key to management is avoidance of silica exposure. Despite this, many develop progressive disease and there are no routinely recommended treatments. This review provides a summary of the literature pertaining to pharmacological therapies for silicosis and examines the plausibility of success of such treatments given the disease pathogenesis. Recent findings In-vitro and in-vivo models demonstrate potential efficacy for drugs, which target inflammasomes, cytokines, effector cells, fibrosis, autophagy, and oxidation. Summary There is some evidence for potential therapeutic targets in silicosis but limited translation into human studies. Treatment of silicosis likely requires a multimodal approach, and there is considerable cross-talk between pathways; agents that modulate both inflammation, fibrosis, autophagy, and ROS production are likely to be most efficacious.

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Section: Antifibrotic Therapymentioning

confidence: 99%