FDA-approved disulfiram inhibits pyroptosis by blocking gasdermin D pore formation

Hu, Jun; Liu, Xing; Xia, Shiyu; Zhang, Zhibin; Zhang, Ying; Zhao, Jingxia; Ruan, Jianbin; Luo, Xi; Lou, Xiwen; Bai, Yang; Wang, Junhong; Hollingsworth, Louis; Magupalli, Venkat Giri; Zhao, Li; Luo, Hongbo; Kim, Justin; Lieberman, Judy; Wu, Hao

doi:10.1038/s41590-020-0669-6

Cited by 605 publications

(467 citation statements)

References 42 publications

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“…Of great interest is the use of existing drugs for inhibition of NETosis. So, disulfiram , which is used to treat alcoholism, inhibits GSDMD activation and protects mice in the lethal LPS-induced sepsis model [ 109 ]. It should be noted that GSDMD is also a critical component of the pyroptosis program and the authors of the study attribute its effect to the prevention of macrophage pyroptosis.…”

Section: Therapy Of Netosismentioning

confidence: 99%

NETosis: Molecular Mechanisms, Role in Physiology and Pathology

Vorobjeva

Chernyak

2020

Biochemistry Moscow

225

162

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NETosis is a program for formation of neutrophil extracellular traps (NETs), which consist of modified chromatin decorated with bactericidal proteins from granules and cytoplasm. Various pathogens, antibodies and immune complexes, cytokines, microcrystals, and other physiological stimuli can cause NETosis. Induction of NETosis depends on reactive oxygen species (ROS), the main source of which is NADPH oxidase. Activation of NADPH oxidase depends on increase in the concentration of Ca 2+ in the cytoplasm and in some cases on the generation of ROS in mitochondria. NETosis includes release of the granule components into the cytosol, modification of histones leading to chromatin decondensation, destruction of the nuclear envelope, as well as formation of pores in the plasma membrane. In this review, basic mechanisms of NETosis, as well as its role in the pathogenesis of some diseases including COVID-19 are discussed.

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Section: Therapy Of Netosismentioning

confidence: 99%

NETosis: Molecular Mechanisms, Role in Physiology and Pathology

Vorobjeva

Chernyak

2020

Biochemistry Moscow

225

162

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“…LDC7559 inhibited pyroptosis by the NLRP3 and AIM2 inflammasomes, 153 but other findings suggest that it may lack activity on recombinant GSDMD in the liposome leakage assay. 160 Future studies should shed light on this apparent paradox.…”

Section: G S Dmd -The Ne W K Id On the B Lo Ckmentioning

confidence: 99%

Therapeutic modulation of inflammasome pathways

Chauhan

Walle

Lamkanfi

2020

Immunological Reviews

137

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Inflammasomes are macromolecular complexes formed in response to pathogen‐associated molecular patterns (PAMPs) and danger‐associated molecular patterns (DAMPs) that drive maturation of the pro‐inflammatory cytokines interleukin (IL)‐1β and IL‐18, and cleave gasdermin D (GSDMD) for induction of pyroptosis. Inflammasomes are highly important in protecting the host from various microbial pathogens and sterile insults. Inflammasome pathways are strictly regulated at both transcriptional and post‐translational checkpoints. When these checkpoints are not properly imposed, undue inflammasome activation may promote inflammatory, metabolic and oncogenic processes that give rise to autoinflammatory, autoimmune, metabolic and malignant diseases. In addition to clinically approved IL‐1‐targeted biologics, upstream targeting of inflammasome pathways recently gained interest as a novel pharmacological strategy for selectively modulating inflammasome activation in pathological conditions.

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“…These mechanisms could be related to the recently discovered ability of disulfiram to block the final step in inflammasome-mediated pyroptosis and cytokine release. 67 Disulfiram blocks gasdermin D (GSDMD), a pore-forming protein that plays a critical role in the terminal step of inflammasome-mediated pathways by facilitating the release of proinflammatory cytokines. [68][69][70] Cleaved GSDMD similarly creates pores on the cell membrane of neutrophils to allow for the release of neutrophil extracellular traps (NETs), a process known as NETosis.…”

Section: Discussionmentioning

confidence: 99%

“…58,73,74 Disulfiram has already been shown to protect mice from lethal lipopolysaccharide-induced septic shock. 67 There is mounting evidence that targeting NETosis and inflammasome activation could be a potential treatment for severe COVID-19. Markers in the sera of patients with severe COVID-19 indicate the presence of NETs, and an autopsy of a lung specimen from a patient with COVID-19 showed extensive neutrophil infiltration.…”

Section: Discussionmentioning

confidence: 99%

A Multi-Phenotype System to Discover Therapies for Age-Related Dysregulation of the Immune Response to Viral Infections

White

Komalo

Nicolaisen

et al. 2020

Preprint

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Age-related immune dysregulation contributes to increased susceptibility to infection and disease in older adults. We combined high-throughput laboratory automation with machine learning to build a multi-phenotype aging profile that models the dysfunctional immune response to viral infection in older adults. From a single well, our multi-phenotype aging profile can capture changes in cell composition, physical cell-to-cell interaction, organelle structure, cytokines, and other hidden complexities contributing to age-related dysfunction. This system allows for rapid identification of new potential compounds to rejuvenate older adults’ immune response. We used our technology to screen thousands of compounds for their ability to make old immune cells respond to viral infection like young immune cells. We observed beneficial effects of multiple compounds, of which two of the most promising were disulfiram and triptonide. Our findings indicate that disulfiram could be considered as a treatment for severe coronavirus disease 2019 and other inflammatory infections.

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FDA-approved disulfiram inhibits pyroptosis by blocking gasdermin D pore formation

Cited by 605 publications

References 42 publications

NETosis: Molecular Mechanisms, Role in Physiology and Pathology

NETosis: Molecular Mechanisms, Role in Physiology and Pathology

Therapeutic modulation of inflammasome pathways

A Multi-Phenotype System to Discover Therapies for Age-Related Dysregulation of the Immune Response to Viral Infections

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