Peroxiredoxin 3 Inhibits Acetaminophen-Induced Liver Pyroptosis Through the Regulation of Mitochondrial ROS

Wang, Yue; Zhao, Yan; Wang, Zhecheng; Sun, Ruimin; Zou, Boyang; Li, Ruixi; Liu, Deshun; Lin, Musen; Zhou, Jiren; Ning, Shili; Tian, Xiaofeng; Yao, Jihong

doi:10.3389/fimmu.2021.652782

Cited by 39 publications

(49 citation statements)

References 58 publications

(86 reference statements)

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“…Prxs are well-known antioxidant proteins that scavenge peroxides in cells. In this aspect, many studies demonstrated that Prxs could play a protective role in diverse disease models ( 24 25 26 27 28 ). Recent evidence has suggested that Prxs could possibly act as DAMP molecules mediating the secretion of inflammatory cytokines as shown in various disease models ( 1 6 7 8 ).…”

Section: Discussionmentioning

confidence: 99%

Inflammasome-Dependent Peroxiredoxin 2 Secretion Induces the Classical Complement Pathway Activation

et al. 2021

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Section: Discussionmentioning

confidence: 99%

Inflammasome-Dependent Peroxiredoxin 2 Secretion Induces the Classical Complement Pathway Activation

et al. 2021

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“…The excessive amounts of glutathione needed to eliminate toxic NAPQI results in oxidative stress in cells, which finally leads to mitochondrial dysfunction, inflammasome activation, and cell death through apoptosis as well as pyroptosis [ 89 ]. Wang, et al studied animal models of drug-induced acute liver injury caused by the intraperitoneal administration of APAP or carbon tetrachloride, and found the processing of GSDMD into its p30 pore forming fragment, procaspase-1 into its p20 active fragment, and pro-IL-1β into its mature form, suggesting inflammasome-dependent pyroptosis in APAP-induced acute liver injury [ 90 ]. The activation of inflammasome-dependent pyroptosis by APAP was also observed in primary cultures of hepatocytes as well as Kupffer cells, indicating that both liver parenchymal cells and immune cells contribute to acute liver injury [ 90 ].…”

Section: Prdxsmentioning

confidence: 99%

“…Wang, et al studied animal models of drug-induced acute liver injury caused by the intraperitoneal administration of APAP or carbon tetrachloride, and found the processing of GSDMD into its p30 pore forming fragment, procaspase-1 into its p20 active fragment, and pro-IL-1β into its mature form, suggesting inflammasome-dependent pyroptosis in APAP-induced acute liver injury [ 90 ]. The activation of inflammasome-dependent pyroptosis by APAP was also observed in primary cultures of hepatocytes as well as Kupffer cells, indicating that both liver parenchymal cells and immune cells contribute to acute liver injury [ 90 ]. They also demonstrated that APAP-induced liver pyroptosis could be ameliorated and reduced by the siRNAs for NLRP3 and Prdx3, showing that liver injury by APAP is dependent on NLRP3 inflammasomes and negatively regulated by Prdx3 [ 90 ].…”

Section: Prdxsmentioning

confidence: 99%

“…The activation of inflammasome-dependent pyroptosis by APAP was also observed in primary cultures of hepatocytes as well as Kupffer cells, indicating that both liver parenchymal cells and immune cells contribute to acute liver injury [ 90 ]. They also demonstrated that APAP-induced liver pyroptosis could be ameliorated and reduced by the siRNAs for NLRP3 and Prdx3, showing that liver injury by APAP is dependent on NLRP3 inflammasomes and negatively regulated by Prdx3 [ 90 ]. The negative regulation of NLRP3 inflammasomes by Prdx3 is cancelled by a scavenger of mitochondrial ROS (Mito-TEMPO) [ 90 ].…”

Section: Prdxsmentioning

confidence: 99%

“…They also demonstrated that APAP-induced liver pyroptosis could be ameliorated and reduced by the siRNAs for NLRP3 and Prdx3, showing that liver injury by APAP is dependent on NLRP3 inflammasomes and negatively regulated by Prdx3 [ 90 ]. The negative regulation of NLRP3 inflammasomes by Prdx3 is cancelled by a scavenger of mitochondrial ROS (Mito-TEMPO) [ 90 ]. Prdx3 knock-out was found to increase mitochondrial ROS, indicating that Prdx3 negatively regulates NLRP3 activation through its antioxidative effects on mitochondria [ 90 ] ( Figure 6 ).…”

Section: Prdxsmentioning

confidence: 99%

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The Role of Peroxiredoxins in the Regulation of Sepsis

2022

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Oxidative stress, a result of a disturbance in redox homeostasis, is considered to be one of the main aggravating events in the pathogenesis of immune disorders. Peroxiredoxins (Prdxs) are an enzyme family that catalyzes the reduction of peroxides, including hydrogen peroxide, lipid peroxides, and nitrogen peroxides. Although the maintenance of cellular redox homeostasis through Prdxs is essential for surviving in adverse environments, Prdxs also participate in the regulation of cellular signal transduction by modulating the activities of a panel of molecules involved in the signal transduction process. Although Prdxs were discovered as intracellular anti-oxidative enzymes, recent research has revealed that Prdxs also play important roles in the extracellular milieu. Indeed, Prdxs have been shown to have the capacity to activate immune cells through ligation with innate immune receptors such as toll-like receptors (TLRs). In this review, we will summarize the intracellular as well as extracellular roles of Prdxs for and against the pathogenesis of inflammatory disorders including sepsis, hemorrhagic shock, and drug-induced liver injury.

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Mitochondrial‐Targeted Delivery of Polyphenol‐Mediated Antioxidases Complexes against Pyroptosis and Inflammatory Diseases

Zhang

Gao

et al. 2023

Advanced Materials

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Excess accumulation of mitochondrial reactive oxygen species (mtROS) is a key target for inhibiting pyroptosis‐induced inflammation and tissue damage. However, targeted delivery of drugs to mitochondria and efficient clearance of mtROS remain challenging. In current study, it is discovered that polyphenols such as tannic acid (TA) can mediate the targeting of polyphenol/antioxidases complexes to mitochondria. This affinity does not depend on mitochondrial membrane potential but stems from the strong binding of TA to mitochondrial outer membrane proteins. Taking advantage of the feasibility of self‐assembly between TA and proteins, superoxide dismutase, catalase, and TA are assembled into complexes (referred to as TSC) for efficient enzymatic activity maintenance. In vitro fluorescence confocal imaging shows that TSC not only promoted the uptake of biological enzymes in hepatocytes but also highly overlapped with mitochondria after lysosomal escape. The results from an in vitro model of hepatocyte oxidative stress demonstrate that TSC efficiently scavenges excess mtROS and reverses mitochondrial depolarization, thereby inhibiting inflammasome‐mediated pyroptosis. More interestingly, TSC maintain superior efficacy compared with the clinical gold standard drug N‐acetylcysteine in both acetaminophen‐ and D‐galactosamine/lipopolysaccharide‐induced pyroptosis‐related hepatitis mouse models. In conclusion, this study opens a new paradigm for targeting mitochondrial oxidative stress to inhibit pyroptosis and treat inflammatory diseases.

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Peroxiredoxin 3 Inhibits Acetaminophen-Induced Liver Pyroptosis Through the Regulation of Mitochondrial ROS

Cited by 39 publications

References 58 publications

Inflammasome-Dependent Peroxiredoxin 2 Secretion Induces the Classical Complement Pathway Activation

Inflammasome-Dependent Peroxiredoxin 2 Secretion Induces the Classical Complement Pathway Activation

The Role of Peroxiredoxins in the Regulation of Sepsis

Mitochondrial‐Targeted Delivery of Polyphenol‐Mediated Antioxidases Complexes against Pyroptosis and Inflammatory Diseases

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