Your search keyword '"INFLAMMASOMES"' showing total 20,090 results

1. Rhein targets macrophage SIRT2 to promote adipose tissue thermogenesis in obesity in mice.

Author

Zhou, Ruo-Nan, Zhu, Zi-Wei, Xu, Ping-Yuan, Shen, Li-Xuan, Wang, Ziwei, Xue, Ying-Ying, Xiang, Ying-Ying, Cao, Yue, Yu, Xi-Zhong, Zhao, Juan, Jin, Yu, Yan, Jing, Yang, Qin, Fang, Peng-Hua, and Shang, Wen-Bin

Subjects

Animals, Male, Mice, Adipocytes, Adipose Tissue, Anthraquinones, Inflammasomes, Macrophages, Mice, Inbred C57BL, NLR Family, Pyrin Domain-Containing 3 Protein, Obesity, Sirtuin 2, Thermogenesis

Abstract

Rhein, a component derived from rhubarb, has been proven to possess anti-inflammatory properties. Here, we show that rhein mitigates obesity by promoting adipose tissue thermogenesis in diet-induced obese mice. We construct a macrophage-adipocyte co-culture system and demonstrate that rhein promotes adipocyte thermogenesis through inhibiting NLRP3 inflammasome activation in macrophages. Moreover, clues from acetylome analysis identify SIRT2 as a potential drug target of rhein. We further verify that rhein directly interacts with SIRT2 and inhibits NLRP3 inflammasome activation in a SIRT2-dependent way. Myeloid knockdown of SIRT2 abrogates adipose tissue thermogenesis and metabolic benefits in obese mice induced by rhein. Together, our findings elucidate that rhein inhibits NLRP3 inflammasome activation in macrophages by regulating SIRT2, and thus promotes white adipose tissue thermogenesis during obesity. These findings uncover the molecular mechanism underlying the anti-inflammatory and anti-obesity effects of rhein, and suggest that rhein may become a potential drug for treating obesity.

Published

2024

2. The inflammasome pathway is activated by dengue virus non-structural protein 1 and is protective during dengue virus infection.

Author

Wong, Marcus, Juan, Evan, Pahmeier, Felix, Chelluri, Sai, Wang, Phoebe, Castillo-Rojas, Bryan, Blanc, Sophie, Vance, Russell, Harris, Eva, and Biering, Scott

Subjects

Viral Nonstructural Proteins, Animals, Inflammasomes, Dengue, Mice, Dengue Virus, Humans, Macrophages, Interleukin-1beta, Mice, Inbred C57BL, Mice, Knockout, Caspase 1

Abstract

Dengue virus (DENV) is a medically important flavivirus causing an estimated 50-100 million dengue cases annually, some of whom progress to severe disease. DENV non-structural protein 1 (NS1) is secreted from infected cells and has been implicated as a major driver of dengue pathogenesis by inducing endothelial barrier dysfunction. However, less is known about how DENV NS1 interacts with immune cells and what role these interactions play. Here we report that DENV NS1 can trigger activation of inflammasomes, a family of cytosolic innate immune sensors that respond to infectious and noxious stimuli, in mouse and human macrophages. DENV NS1 induces the release of IL-1β in a caspase-1 dependent manner. Additionally, we find that DENV NS1-induced inflammasome activation is independent of the NLRP3, Pyrin, and AIM2 inflammasome pathways, but requires CD14. Intriguingly, DENV NS1-induced inflammasome activation does not induce pyroptosis and rapid cell death; instead, macrophages maintain cellular viability while releasing IL-1β. Lastly, we show that caspase-1/11-deficient, but not NLRP3-deficient, mice are more susceptible to lethal DENV infection. Together, these results indicate that the inflammasome pathway acts as a sensor of DENV NS1 and plays a protective role during infection.

Published

2024

3. Host E3 ubiquitin ligase ITCH mediates Toxoplasma gondii effector GRA35-triggered NLRP1 inflammasome activation and cell-autonomous immunity

Author

Wang, Yifan, Hollingsworth, L Robert, Sangaré, Lamba Omar, Paredes-Santos, Tatiana C, Krishnamurthy, Shruthi, Penn, Bennett H, Wu, Hao, and Saeij, Jeroen PJ

Subjects

Biochemistry and Cell Biology, Biological Sciences, Foodborne Illness, Vaccine Related, Biodefense, Infectious Diseases, Emerging Infectious Diseases, Prevention, 2.2 Factors relating to the physical environment, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Infection, Animals, Humans, Rats, Adenosine Triphosphatases, Immunity, Innate, Inflammasomes, NLR Proteins, Protozoan Proteins, Rats, Inbred Lew, Toxoplasma, Ubiquitin-Protein Ligases, E3 ubiquitin ligase, effector-triggered immunity, NLRP1 inflammasome, IFN gamma, Toxoplasma gondii, IFNγ, Microbiology, Biochemistry and cell biology, Medical microbiology

Abstract

Toxoplasma gondii is an intracellular parasite that can activate the NLRP1 inflammasome leading to macrophage pyroptosis in Lewis rats, but the underlying mechanism is not well understood. In this study, we performed a genome-wide CRISPR screen and identified the dense granule proteins GRA35, GRA42, and GRA43 as the Toxoplasma effectors mediating cell death in Lewis rat macrophages. GRA35 localizes on the parasitophorous vacuole membrane, where it interacts with the host E3 ubiquitin ligase ITCH. Inhibition of proteasome activity or ITCH knockout prevented pyroptosis in Toxoplasma-infected Lewis rat macrophages, consistent with the "NLRP1 functional degradation model." However, there was no evidence that ITCH directly ubiquitinates or interacts with rat NLRP1. We also found that GRA35-ITCH interaction affected Toxoplasma fitness in IFNγ-activated human fibroblasts, likely due to ITCH's role in recruiting ubiquitin and the parasite-restriction factor RNF213 to the parasitophorous vacuole membrane. These findings identify a new role of host E3 ubiquitin ligase ITCH in mediating effector-triggered immunity, a critical concept that involves recognizing intracellular pathogens and initiating host innate immune responses.IMPORTANCEEffector-triggered immunity represents an innate immune defense mechanism that plays a crucial role in sensing and controlling intracellular pathogen infection. The NLRP1 inflammasome in the Lewis rats can detect Toxoplasma infection, which triggers proptosis in infected macrophages and eliminates the parasite's replication niche. The work reported here revealed that host E3 ubiquitin ligase ITCH is able to recognize and interact with Toxoplasma effector protein GRA35 localized on the parasite-host interface, leading to NLRP1 inflammasome activation in Lewis rat macrophages. Furthermore, ITCH-GRA35 interaction contributes to the restriction of Toxoplasma in human fibroblasts stimulated by IFNγ. Thus, this research provides valuable insights into understanding pathogen recognition and restriction mediated by host E3 ubiquitin ligase.

Published

2024

4. Diacylglycerols and Lysophosphatidic Acid, Enriched on Lipoprotein(a), Contribute to Monocyte Inflammation.

Author

Dzobo, Kim, Cupido, Arjen, Mol, Barend, Stiekema, Lotte, Versloot, Miranda, Winkelmeijer, Maaike, Peter, Jorge, Pennekamp, Anne-Marije, Havik, Stefan, Vaz, Frédéric, van Weeghel, Michel, Prange, Koen, Levels, Johannes, de Winther, Menno, Tsimikas, Sotirios, Groen, Albert, Stroes, Erik, de Kleijn, Dominique, and Kroon, Jeffrey

Subjects

diglycerides, inflammation, lipidomics, lipoprotein(a), monocytes, Humans, Diglycerides, Inflammasomes, Inflammation, Interleukin-1beta, Interleukin-6, Lipoprotein(a), Lysophospholipids, Monocytes, NF-kappa B, NLR Family, Pyrin Domain-Containing 3 Protein

Abstract

BACKGROUND: Oxidized phospholipids play a key role in the atherogenic potential of lipoprotein(a) (Lp[a]); however, Lp(a) is a complex particle that warrants research into additional proinflammatory mediators. We hypothesized that additional Lp(a)-associated lipids contribute to the atherogenicity of Lp(a). METHODS: Untargeted lipidomics was performed on plasma and isolated lipoprotein fractions. The atherogenicity of the observed Lp(a)-associated lipids was tested ex vivo in primary human monocytes by RNA sequencing, ELISA, Western blot, and transendothelial migratory assays. Using immunofluorescence staining and single-cell RNA sequencing, the phenotype of macrophages was investigated in human atherosclerotic lesions. RESULTS: Compared with healthy individuals with low/normal Lp(a) levels (median, 7 mg/dL [18 nmol/L]; n=13), individuals with elevated Lp(a) levels (median, 87 mg/dL [218 nmol/L]; n=12) demonstrated an increase in lipid species, particularly diacylglycerols (DGs) and lysophosphatidic acid (LPA). DG and the LPA precursor lysophosphatidylcholine were enriched in the Lp(a) fraction. Ex vivo stimulation with DG(40:6) demonstrated a significant upregulation in proinflammatory pathways related to leukocyte migration, chemotaxis, NF-κB (nuclear factor kappa B) signaling, and cytokine production. Functional assessment showed a dose-dependent increase in the secretion of IL (interleukin)-6, IL-8, and IL-1β after DG(40:6) and DG(38:4) stimulation, which was, in part, mediated via the NLRP3 (NOD [nucleotide-binding oligomerization domain]-like receptor family pyrin domain containing 3) inflammasome. Conversely, LPA-stimulated monocytes did not exhibit an inflammatory phenotype. Furthermore, activation of monocytes by DGs and LPA increased their transendothelial migratory capacity. Human atherosclerotic plaques from patients with high Lp(a) levels demonstrated colocalization of Lp(a) with M1 macrophages, and an enrichment of CD68+IL-18+TLR4+ (toll-like receptor) TREM2+ (triggering receptor expressed on myeloid cells) resident macrophages and CD68+CASP1+ (caspase) IL-1B+SELL+ (selectin L) inflammatory macrophages compared with patients with low Lp(a). Finally, potent Lp(a)-lowering treatment (pelacarsen) resulted in a reduction in specific circulating DG lipid subspecies in patients with cardiovascular disease with elevated Lp(a) levels (median, 82 mg/dL [205 nmol/L]). CONCLUSIONS: Lp(a)-associated DGs and LPA have a potential role in Lp(a)-induced monocyte inflammation by increasing cytokine secretion and monocyte transendothelial migration. This DG-induced inflammation is, in part, NLRP3 inflammasome dependent.

Published

2024

5. The discovery of NLRP3 and its function in cryopyrin‐associated periodic syndromes and innate immunity

Author

Putnam, Christopher D, Broderick, Lori, and Hoffman, Hal M

Subjects

Biomedical and Clinical Sciences, Immunology, Clinical Research, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Humans, Mice, Animals, NLR Family, Pyrin Domain-Containing 3 Protein, Cryopyrin-Associated Periodic Syndromes, Inflammasomes, Immunity, Innate, Inflammation, Interleukin-1beta, cryopyrin-associated periodic syndrome, familial cold autoinflammatory syndrome, inflammasome, NLRP3, Cryopyrin-associated Periodic Syndromes

Abstract

From studies of individual families to global collaborative efforts, the NLRP3 inflammasome is now recognized to be a key regulator of innate immunity. Activated by a panoply of pathogen-associated and endogenous triggers, NLRP3 serves as an intracellular sensor that drives carefully coordinated assembly of the inflammasome, and downstream inflammation mediated by IL-1 and IL-18. Initially discovered as the cause of the autoinflammatory spectrum of cryopyrin-associated periodic syndrome (CAPS), NLRP3 is now also known to play a role in more common diseases including cardiovascular disease, gout, and liver disease. We have seen cohesion in results from clinical studies in CAPS patients, ex vivo studies of human cells and murine cells, and in vivo murine models leading to our understanding of the downstream pathways, cytokine secretion, and cell death pathways that has solidified the role of autoinflammation in the pathogenesis of human disease. Recent advances in our understanding of the structure of the inflammasome have provided ways for us to visualize normal and mutant protein function and pharmacologic inhibition. The subsequent development of targeted therapies successfully used in the treatment of patients with CAPS completes the bench to bedside translational loop which has defined the study of this unique protein.

Published

2024

6. Extracorporeal Shockwave Therapy Alleviates Inflammatory Pain by Down-Regulating NLRP3 Inflammasome in Experimental Chronic Prostatitis and Chronic Pelvic Pain Syndrome.

Author

Bae, Woong, Shin, Dongho, Piao, Jun, Kim, Soomin, Choi, Yong, Park, Bong, Jung, Hyun, Sorkhi, Samuel, Chawla, Saager, Cheon, Chung, Kang, Dae, Choi, Jong, Park, Sang-Hyuck, Kim, Sae, and Rajasekaran, Mahadevan

Subjects

Apoptosis, Extracorporeal shockwave therapy, Inflammasomes, Prostatitis

Abstract

PURPOSE: To evaluate the anti-inflammatory and antioxidative effects of extracorporeal shockwave therapy (ESWT) on prostatitis and explore the mechanism of alleviating pain. MATERIALS AND METHODS: For in vitro testing, RWPE-1 cells were randomly divided into 5 groups: (1) RWPE-1 group (normal control), (2) LPS group (lipopolysaccharide inducing inflammation), (3) 0.1ESWT group (treated by 0.1 mJ/mm² energy level), (4) 0.2ESWT group (treated by 0.2 mJ/mm² energy level), and (5) 0.3ESWT group (treated by 0.3 mJ/mm² energy level). After ESWT was administered, cells and supernatant were collected for ELISA and western blot. For in vivo testing, Sprague-Dawley male rats were randomly divided into 3 groups: (1) normal group, (2) prostatitis group, and (3) ESWT group (n=12 for each). Prostatitis was induced by 17 beta-estradiol and dihydrotestosterone (DHT) administration. Four weeks after ESWT, the pain index was assessed for all groups and prostate tissues were collected for immunohistochemistry, immunofluorescence, apoptosis analysis and, western blot. RESULTS: Our in vitro studies showed that the optimal energy flux density of ESWT was 0.2 mJ/mm². In vivo, ESWT ameliorated discomfort in rats with prostatitis and inflammation symptoms were improved. Compared to normal rats, overexpressed NLRP3 inflammasomes triggered apoptosis in rats with prostatitis and this was improved by ESWT. TLR4-NFκB pathway was overactive after experimental prostatitis, compared to normal and ESWT groups, and prostatitis induced alterations in BAX/BAK pathway were inhibited by ESWT. CONCLUSIONS: ESWT improved CP/CPPS by reducing NLRP3 inflammasome and ameliorated apoptosis via inhibiting BAX/BAK pathway in a rat model. TLR4 may play a key role in bonding NLRP3 inflammasome and BAX/BAK pathways. ESWT might be a promising approach for the treatment of CP/CPPS.

Published

2024

7. Inflammasomes: emerging therapeutic targets in hidradenitis suppurativa?

Author

Campbell, Ciara, Mayatra, Jay M, Neve, Ashish J, Fletcher, Jean M, and Johnston, Daniel G W

Subjects

*INFLAMMASOMES, *HAIR follicles, *SKIN diseases, *DRUG target, *INTERLEUKIN-17

Abstract

Hidradenitis suppurativa (HS) is a chronic inflammatory skin disease characterized by recurrent inflammatory lesions, which affect skin and hair follicles in intertriginous areas. HS has a multifactorial aetiology resulting in barrier dysfunction associated with aberrant immune activation. There is increased evidence for the role of inflammasomes in the pathophysiology of inflammatory skin diseases, including HS. Inflammasomes are multiprotein complexes activated following exposure to danger signals, including microbial ligands and components of damaged host cells. Inflammasome activation induces many signalling cascades and subsequent cleavage of proinflammatory cytokines – most notably interleukin (IL)-1β – which have a role in HS pathogenesis. Limited immunotherapies are approved for treating moderate-to-severe HS, with variable response rates influenced by disease heterogeneity. Inflammasomes represent attractive targets to suppress multiple inflammatory pathways in HS, including IL-1β and IL-17. This review aims to summarize the role of inflammasomes in HS and to evaluate evidence for inflammasomes as therapeutic targets for HS treatment. [ABSTRACT FROM AUTHOR]

Published

2024

8. Discovery, Total Synthesis, and Anti‐Inflammatory Evaluation of Naturally Occurring Naphthopyrone‐Macrolide Hybrids as Potent NLRP3 Inflammasome Inhibitors.

Author

Sun, Chunxiao, Jiang, Yuqi, Li, Changlong, Sun, Simin, Lin, Jiaqi, Wang, Wenxue, Zhou, Luning, Li, Liping, Shah, Mudassir, Che, Qian, Zhang, Guojian, Wang, De, Zhu, Tianjiao, and Li, Dehai

Subjects

*BIOMIMETIC synthesis, *BIOLOGICAL assay, *NLRP3 protein, *LEAD compounds, *INFLAMMASOMES

Abstract

Numerous clinical disorders have been linked to the etiology of dysregulated NLRP3 (NACHT, LRR, and PYD domain‐containing protein 3) inflammasome activation. Despite its potential as a pharmacological target, modulation of NLRP3 activity remains challenging. Only a sparse number of compounds have been reported that can modulate NLRP3 and none of them have been developed into a commercially available drug. In this research, we identified three potent NLRP3 inflammasome inhibitors, gymnoasins A‐C (1–3), with unprecedented pentacyclic scaffolds, from an Antarctic fungus Pseudogymnoascus sp. HDN17‐895, which represent the first naturally occurring naphthopyrone‐macrolide hybrids. Additionally, biomimetic synthesis of gymnoasin A (1) was also achieved validating the chemical structure and affording ample amounts of material for exhaustive bioactivity assessments. Biological assays indicated that 1 could significantly inhibited in vitro NLRP3 inflammasome activation and in vivo pro‐inflammatory cytokine IL‐1β release, representing a valuable new lead compound for the development of novel therapeutics with the potential to inhibit the NLRP3 inflammasome. [ABSTRACT FROM AUTHOR]

Published

2024

9. Cytoplasmic DNA and AIM2 inflammasome in RA: where they come from and where they go?

Author

Conghui Xu, Weiyao Jing, Cui Liu, Bo Yuan, Xinghua Zhang, Limei Liu, Fengfan Zhang, Ping Chen, Qiang Liu, Haidong Wang, and Xiaozheng Du

Subjects

RHEUMATOID arthritis, AUTOIMMUNE diseases, ETIOLOGY of diseases, CELLULAR signal transduction, INFLAMMASOMES

Abstract

Rheumatoid arthritis is a chronic autoimmune disease of undetermined etiology characterized by symmetric synovitis with predominantly destructive and multiple joint inflammation. Cytoplasmic DNA sensors that recognize protein molecules that are not themselves or abnormal dsDNA fragments play an integral role in the generation and perpetuation of autoimmune diseases by activating different signaling pathways and triggering innate immune signaling pathways and host defenses. Among them, melanoma deficiency factor 2 (AIM2) recognizes damaged DNA and double-stranded DNA and binds to them to further assemble inflammasome, initiating the innate immune response and participating in the pathophysiological process of rheumatoid arthritis. In this article, we review the research progress on the source of cytoplasmic DNA, the mechanism of assembly and activation of AIM2 inflammasome, and the related roles of other cytoplasmic DNA sensors in rheumatoid arthritis. [ABSTRACT FROM AUTHOR]

Published

2024

10. Regulation of the NLRP3 inflammasome by autophagy and mitophagy.

Author

Gupta, Suman, Cassel, Suzanne L., Sutterwala, Fayyaz S., and Dagvadorj, Jargalsaikhan

Subjects

*NLRP3 protein, *INFLAMMASOMES, *LUNG diseases, *PULMONARY manifestations of general diseases, *INFLAMMATION

Abstract

Summary The NLRP3 inflammasome is a multiprotein complex that upon activation by the innate immune system drives a broad inflammatory response. The primary initial mediators of this response are pro‐IL‐1β and pro‐IL‐18, both of which are in an inactive form. Formation and activation of the NLRP3 inflammasome activates caspase‐1, which cleaves pro‐IL‐1β and pro‐IL‐18 and triggers the formation of gasdermin D pores. Gasdermin D pores allow for the secretion of active IL‐1β and IL‐18 initiating the organism‐wide inflammatory response. The NLRP3 inflammasome response can be beneficial to the host; however, if the NLRP3 inflammasome is inappropriately activated it can lead to significant pathology. While the primary components of the NLRP3 inflammasome are known, the precise details of assembly and activation are less well defined and conflicting. Here, we discuss several of the proposed pathways of activation of the NLRP3 inflammasome. We examine the role of subcellular localization and the reciprocal regulation of the NLRP3 inflammasome by autophagy. We focus on the roles of mitochondria and mitophagy in activating and regulating the NLRP3 inflammasome. Finally, we detail the impact of pathologic NLRP3 responses in the development and manifestations of pulmonary disease. [ABSTRACT FROM AUTHOR]

Published

2024

11. Sprayable inflammasome-inhibiting lipid nanorods in a polymeric scaffold for psoriasis therapy.

Author

Surve, Dhanashree, Fish, Adam, Debnath, Maharshi, Pinjari, Aniruddha, Lorenzana, Adrian, Piya, Sumi, Peyton, Shelly, and Kulkarni, Ashish

Subjects

REACTIVE oxygen species, NANORODS, INFLAMMASOMES, NLRP3 protein, CASPASES

Abstract

Localized delivery of inflammasome inhibitors in phagocytic macrophages could be promising for psoriasis treatment. The present work demonstrates the development of non-spherical lipid nanoparticles, mimicking pathogen-like shapes, consisting of an anti-inflammatory inflammasome inhibiting lipid (pyridoxine dipalmitate) as a trojan horse. The nanorods inhibit inflammasome by 3.8- and 4.5-fold compared with nanoellipses and nanospheres, respectively. Nanorods reduce apoptosis-associated speck-like protein and lysosomal rupture, restrain calcium influx, and mitochondrial reactive oxygen species. Dual inflammasome inhibitor (NLRP3/AIM-2-IN-3) loaded nanorods cause synergistic inhibition by 21.5- and 59-folds compared with nanorods and free drug, respectively alongside caspase-1 inhibition. The NLRP3/AIM-2-IN-3 nanorod when transformed into a polymeric scaffold, simultaneously and effectively inhibits RNA levels of NLRP3, AIM2, caspase-1, chemokine ligand-2, gasdermin-D, interleukin-1β, toll-like receptor 7/ 8, and IL-17A by 6.4-, 1.6-, 2.0-, 13.0-, 4.2-, 24.4-, 4.3-, and 1.82-fold, respectively in psoriatic skin in comparison to Imiquimod positive control group in an in-vivo psoriasis-like mice model. Inflammasome inhibitors have potential in psoriasis treatment. Here, the authors report on a study into the shape effects of non-spherical anti-inflammatory lipid nanoparticles made from inflammasome inhibiting lipid and demonstrate application in reducing inflammasome formation in psoriasis in vivo models. [ABSTRACT FROM AUTHOR]

Published

2024

12. Genetic and epigenetic dysregulation of innate immune mechanisms in autoinflammatory diseases.

Author

Merlo Pich, Laura M., Ziogas, Athanasios, and Netea, Mihai G.

Subjects

*AUTOINFLAMMATORY diseases, *IMMUNE response, *IMMUNE system, *INTERFERONS, *INFLAMMASOMES

Abstract

Dysregulation and hyperactivation of innate immune responses can lead to the onset of systemic autoinflammatory diseases. Monogenic autoinflammatory diseases are caused by inborn genetic errors and based on molecular mechanisms at play, can be divided into inflammasomopathies, interferonopathies, relopathies, protein misfolding, and endogenous antagonist deficiencies. On the other hand, more common autoinflammatory diseases are multifactorial, with both genetic and non‐genetic factors playing an important role. During the last decade, long‐term memory characteristics of innate immune responses have been described (also called trained immunity) that in physiological conditions provide enhanced host protection from pathogenic re‐infection. However, if dysregulated, induction of trained immunity can become maladaptive, perpetuating chronic inflammatory activation. Here, we describe the mechanisms of genetic and epigenetic dysregulation of the innate immune system and maladaptive trained immunity that leads to the onset and perpetuation of the most common and recently described systemic autoinflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2024

13. Autophagy and inflammasome activation are associated with poor response to FLT3 inhibitors in patients with FLT3-ITD acute myeloid leukemia.

Author

Santos de Macedo, Brunno Gilberto, Albuquerque de Melo, Manuela, Pereira-Martins, Diego Antonio, Machado-Neto, João Agostinho, and Traina, Fabíola

Subjects

*ACUTE myeloid leukemia, *INFLAMMASOMES, *DRUG resistance, *AUTOPHAGY, *SORAFENIB

Abstract

Beyond its clinical diversity and severity, acute myeloid leukemia (AML) is known for its complex molecular background and for rewiring biological processes to aid disease onset and maintenance. FLT3 mutations are among the most recurring molecular entities that cooperatively drive AML, and their inhibition is a critical molecularly oriented therapeutic strategy. Despite being a promising avenue, it still faces challenges such as intrinsic and acquired drug resistance, which led us to investigate whether and how autophagy and inflammasome interact and whether this interaction could be leveraged to enhance FLT3 inhibition as a therapeutic strategy. We observed a strong and positive correlation between the expression of key genes associated with autophagy and the inflammasome. Gene set enrichment analysis of the FLT3-ITD samples and their ex vivo response to five different FLT3 inhibitors revealed a common molecular signature compatible with autophagy and inflammasome activation across all poor responders. Inflammasome activation was also shown to strongly increase the likelihood of a poor ex vivo response to the FLT3 inhibitors quizartinib and sorafenib. These findings reveal a distinct molecular pattern within FLT3-ITD AML samples that underscores the necessity for further exploration into how approaching these supportive parallel yet altered pathways could improve therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2024

14. ASC speck serum concentrations, a component of sterile cellular inflammation, are associated with individual cardiopulmonary capacity.

Author

Kogel, Alexander, Voßhage, Nell, Behzadi, Amirhossein, Laufs, Ulrich, and Fikenzer, Sven

Subjects

EXERCISE tests, BODY composition, HEART beat, INFLAMMASOMES, FLOW cytometry

Abstract

Aims: Exercise-induced cellular stress and sterile inflammation are of increasing interest. ASC specks are a component of the intracellular NLRP3-inflammasome and can be released into the blood. For example, serum ASC specks are increased after marathon running.We therefore tested whether ASC specks are potentially associated with the individual response to physical training and cardiopulmonary capacity. Methods: We performed a prospective study in 45 healthy athletes. Blood samples were taken before and after cardiopulmonary exercise testing (CPET). ASC speck concentrations were quantitated using flow cytometry. Results: Baseline ASC speck levels correlated with clinical parameters of body composition (height, weight, BMI) and parameters of cardiopulmonary performance (peak VO2, peak oxygen pulse, heart rate after exercise). Athletes with lowest baseline ASC speck concentrations have a significantly lower BMI (22.0 ± 1.8 vs. 24.9 ± 1.6 kg/m2), higher heart rate at rest (72 ± 10 vs. 58 ± 10 beats/ min), lower peak VO2 (2692 ± 629 vs. 3404 ± 747 mL/min) and lower peak oxygen pulse (15.6 ± 3.4 vs. 20.7 ± 3.5 mL/heart rate). Overall, ASC speck concentrations showed no significant change after CPET (7.0 ± 4.5 vs. 8.0 ± 5.4 ASC specks/µL, p = 0.3). However, subgroup analysis revealed a significant increase in circulating ASC specks in athletes with the lowest baseline values (2.37 ± 0.84 vs. 8.43 ± 7.52 ASC specks/µL, p < 0.05). Athletes with an increase in ASC speck concentrations in response to CPET had a lower peak oxygen pulse compared to those with a decrease (17.1 ± 4.2 vs. 19.8 ± 4.1, p < 0.05). Conclusion: Low ASC speck baseline values as well as an increase in response to exercise are associated with lower peak oxygen pulse in healthy athletes. [ABSTRACT FROM AUTHOR]

Published

2024

15. Updated insights into the NLRP3 inflammasome in postoperative cognitive dysfunction: emerging mechanisms and treatments.

Author

Tian Wang, Guangwei Sun, and Bingdong Tao

Subjects

MITOCHONDRIAL pathology, COGNITION disorder risk factors, RISK assessment, DISEASE exacerbation, AUTOPHAGY, SURGERY, PATIENTS, HEALTH status indicators, APOPTOSIS, AGE distribution, NEUROINFLAMMATION, CELLULAR signal transduction, OXIDATIVE stress, SURGICAL complications, ATTENTION, COGNITION disorders, SIGNAL peptides, BIOMARKERS, MEMORY disorders, ANESTHESIA, DISEASE progression, NEUROTRANSMITTERS, DISEASE risk factors, DISEASE complications, OLD age

Abstract

Postoperative cognitive dysfunction (POCD) poses a significant threat to patients undergoing anesthesia and surgery, particularly elderly patients. It is characterized by diminished cognitive functions post surgery, such as impaired memory and decreased concentration. The potential risk factors for POCD include age, surgical trauma, anesthetic type, and overall health condition; however, the precise mechanisms underlying POCD remain elusive. Recent studies suggest that neuroinflammation might be a primary pathogenic factor. NOD-, LRR- and pyrin domain-containing protein 3 (NLRP3) inflammasomes are implicated in exacerbating POCD by promoting the release of inflammatory factors and proteins that initiate pyroptosis, further influencing the disease process. The regulation of NLRP3 inflammasome activity, including its activation and degradation, is tightly controlled through multiple pathways and mechanisms. In addition, autophagy, a protective mechanism, regulates the NLRP3 inflammasome to control the progression of POCD. This review reviews recent findings on the role of the NLRP3 inflammasome in POCD pathogenesis and discusses therapeutic strategies aimed at reducing NLRP3 sources, inhibiting cellular pyroptosis, and enhancing autophagy. [ABSTRACT FROM AUTHOR]

Published

2024

16. The NLRP3 inflammasome: Mechanisms of activation, regulation, and role in diseases.

Author

Dadkhah, Mina and Sharifi, Mohammadreza

Subjects

*NLRP3 protein, *REACTIVE oxygen species, *INFLAMMASOMES, *PYROPTOSIS, *IONS

Abstract

Abstract\nPLAIN LANGUAGE SUMMARYBecause of numerous stress signals, intracellular protein complexes are called inflammasomes. They function as catalysts for the proteolytic transformation of pro-interleukin into the active form of interleukin. Inflammasomes can promote a type of cell death process known as pyroptosis. The NLRP3 inflammasome, comprised of the NLRP3 protein, procaspase-1, and ASC, tightly regulates inflammation. The NLRP3 inflammasome is activated by a variety of stimuli, and several molecular and cellular events, such as ion influx, mitochondrial dysfunction, reactive oxygen species production, and lysosomal damage have been shown to trigger its activation. Inflammation plays a major role in almost all types of human diseases. The NLRP3 inflammasome has been the most widely studied and plays an important pathogenic role in various inflammatory pathologies. This review briefly presents the basic features of NLRP3 inflammasome and their mechanisms of activation and regulation. In addition, recent studies report the role of NLRP3 inflammasome in several diseases have been summarized.Because of numerous stress signals, intracellular protein complexes are called inflammasomes. They function as catalysts for the proteolytic transformation of pro-interleukin into the active form of interleukin. Inflammasomes can promote a type of cell death process known as pyroptosis. The NLRP3 inflammasome, comprised of the NLRP3 protein, procaspase-1, and ASC, tightly regulates inflammation. The NLRP3 inflammasome is activated by a variety of stimuli, and several molecular and cellular events, such as ion influx, mitochondrial dysfunction, reactive oxygen species production, and lysosomal damage, have been shown to trigger its activation. Also, NLRP3 inflammasome plays a role in several different diseases. [ABSTRACT FROM AUTHOR]

Published

2024

17. Mechanisms of immune evasion by <italic>Mycobacterium tuberculosis</italic>: the impact of T7SS and cell wall lipids on host defenses.

Author

Malik, Asrar Ahmad, Shariq, Mohd, Sheikh, Javaid Ahmad, Jaiswal, Udyeshita, Fayaz, Haleema, Shrivastava, Gauri, Ehtesham, Nasreen Z., and Hasnain, Seyed E.

Subjects

*PROTEIN transport, *ADENOSINE triphosphatase, *INFLAMMASOMES, *AUTOPHAGY, *LIPIDS, *MYCOBACTERIUM tuberculosis

Abstract

HIGHLIGHTSEmergence of MDR strains exacerbates the TB health crisis.M. tb uses T7SS to disrupt host immune responses.Pathogen counters autophagy, dampening host defense mechanisms.T7SSs critical for protein transport and immune evasion.Understanding T7SSs may lead to new TB therapies. [ABSTRACT FROM AUTHOR]

Published

2024

18. Clinical study of Modified Ermiao Granules activating AIM2 inflammasome-mediated pyroptosis to clear HR-HPV and ameliorate LSIL.

Author

Jie Fu, Qingling Ren, and Yue Han

Subjects

*INFLAMMASOMES, *PAPILLOMAVIRUSES, *CELL death, *APOPTOSIS, *NATURAL immunity

Abstract

This study aimed to examine the efficacy and safety of Modified Ermiao Granules in clearing high-risk human papillomavirus (HR-HPV) and reversing low-grade squamous intraepithelial lesions (LSIL), as well as to examine cervical tissues before and after drug treatment for absent in melanoma (AIM2) inflammasome-mediated pyroptosis. A total of 60 patients with persistent HR-HPV infection and cervical histopathology of the LSIL were randomly divided into control group and observation groups (n = 30 each). Observation group participants received Modified Ermiao Granules orally, whereas the control group received recombinant human interferon α2b vaginal effervescent tablets. After treatment, the observation group had a significantly lower HPV DNA loads than the control group (p < 0.05). Compared with the control group, the observation group had a significantly higher HR-HPV clearance rate (χ² = 4.267, p = 0.039). Accordingly, the LSIL reversal rates were 33.33% and 60.00% in the control and observation groups, respectively (χ² = 4.286, p = 0.038). Both treatments reduced clinical symptoms in patients with HR-HPV with LSIL, but the observation group showed greater improvement (p < 0.05). Control and observation groups expressed AIM2 protein positively at 36.67% and 66.37%, respectively (χ² = 5.406, p < 0.05). Caspase-1, gasdermin D (GSDMD), and interleukin (IL)-1β levels in vaginal douche were significantly higher in the observation group than in the control group (p < 0.05). There was a significant negative correlation between HPV DNA load and AIM2 expression in cervical tissues (rho = -0.493, p < 0.05), with caspase-1 (r = -0.439, p < 0.05), GSDMD (r = -0.508, p<0.05) and IL-1β levels (r = -0.347, p = 0.007) in vaginal douche. In conclusion, the Modified Ermiao Granules effectively cleared persistent HRHPV infections and reversed LSIL, which may be associated with its activating effect on AIM2 inflammasome-mediated pyroptosis. [ABSTRACT FROM AUTHOR]

Published

2024

19. CARD8 polymorphisms among bacterial meningitis patients in North-West Ethiopia.

Author

Belayneh, Meseret, Mengesha, Mesfin, Idosa, Berhane A., Fentaw, Surafel, Moges, Biniyam, Tazu, Zelalem, Assefa, Meseret, Garpenholt, Örjan, Persson, Alexander, Särndahl, Eva, Abate, Ebba, Säll, Olof, and Gelaw, Baye

Subjects

*NEISSERIA meningitidis, *STREPTOCOCCUS pneumoniae, *SYMPTOMS, *GENETIC polymorphisms, *BACTERIAL diseases, *BACTERIAL meningitis, *NEISSERIA

Abstract

Background: The severity of infectious disease outcomes is dependent on the virulence factors of the pathogen and the host immune response. CARD8 is a major regulator of the innate immune proinflammatory response and has been suggested to modulate the host response to common inflammatory diseases. In the present study, the C10X genetic polymorphism in the CARD8 gene was investigated in relation to bacterial meningitis. Methods: A total of 400 clinically suspected meningitis patients hospitalized at the University of Gondar Hospital were enrolled in the study. Cerebrospinal fluid (CSF) and blood samples were collected for laboratory investigations. The collected CSF was cultured, and all the results obtained from the culture were confirmed using direct RT‒PCR. Genotyping of whole-blood samples was performed using a TaqMan assay. The results were compared with apparently healthy controls and with PCR-negative meningitis suspected patients. Results: Of the included patients, 57% were men and the most common clinical signs and symptoms were fever (81%), headache (80%), neck stiffness (76%), nausea (68%), and vomiting (67%). Microbiology culture identified 7 patients with bacterial meningitis caused by Neisseria meningitidis (n = 4) and Streptococcus pneumoniae (n = 3). The RT-PCR revealed 39 positive samples for N. meningitidis (n = 10) and S. pneumoniae (n = 29). A total of 332 whole-blood samples were genotyped with the following results: 151 (45.5%) C10X heterozygotes, 59 (17.7%) C10X homozygotes and 122 (36.7%) wild genotypes. The polymorphic gene carriers among laboratory confirmed, clinically diagnosed meningitis and healthy controls were 23(46%), 246(40%), and 1526(39%), respectively with OR = 1.27 (0.7–2.3) and OR = 1.34 (0.76–2.4). The presence of the C10X polymorphism in the CARD8 gene was more prevalent in suspected meningitis patients than in healthy controls (OR 1.2; 1.00-1.5). Homozygote C10X polymorphic gene carriers were more susceptible to infectious disease. The presence of viable or active bacterial infection was found to be associated with the presence of heterozygous C10X carriers. Conclusions: A greater proportion of C10X in the CARD8 gene in confirmed bacterial meningitis patients and clinically diagnosed meningitis patients than in healthy controls. Homozygote C10X polymorphic gene carriers were more susceptible to infectious disease than heterozygote gene carriers and healthy controls. [ABSTRACT FROM AUTHOR]

Published

2024

20. Vaccinia virus F1L blocks the ribotoxic stress response to subvert ZAKα‐dependent NLRP1 inflammasome activation.

Author

Szymanska, Inga, Bauernfried, Stefan, Komar, Tobias, and Hornung, Veit

Subjects

VACCINIA, VIRUS diseases, GENETIC translation, INFLAMMASOMES, IMMUNE response

Abstract

Inflammasomes are essential for host defense, recognizing foreign or stress signals to trigger immune responses, including maturation of IL‐1 family cytokines and pyroptosis. Here, NLRP1 is emerging as an important sensor of viral infection in barrier tissues. NLRP1 is activated by various stimuli, including viral double‐stranded (ds) RNA, ribotoxic stress, and inhibition of dipeptidyl peptidases 8 and 9 (DPP8/9). However, certain viruses, most notably the vaccinia virus, have evolved strategies to subvert inflammasome activation or effector functions. Using the modified vaccinia virus Ankara (MVA) as a model, we investigated how the vaccinia virus inhibits inflammasome activation. We confirmed that the early gene F1L plays a critical role in inhibiting NLRP1 inflammasome activation. Interestingly, it blocks dsRNA and ribotoxic stress‐dependent NLRP1 activation without affecting its DPP9‐inhibition‐mediated activation. Complementation and loss‐of‐function experiments demonstrated the sufficiency and necessity of F1L in blocking NLRP1 activation. Furthermore, we found that F1L‐deficient, but not wild‐type MVA, induced ZAKα activation. Indeed, an F1L‐deficient virus was found to disrupt protein translation more prominently than an unmodified virus, suggesting that F1L acts in part upstream of ZAKα. These findings underscore the inhibitory role of F1L on NLRP1 inflammasome activation and provide insight into viral evasion of host defenses and the intricate mechanisms of inflammasome activation. [ABSTRACT FROM AUTHOR]

Published

2024

21. Role of caspase-11 non-canonical inflammasomes in retinal ischemia/reperfusion injury.

Author

Wan, Yong, Li, Jiayu, Pu, Jialei, Yang, Jing, Pei, Cheng, and Qi, Yun

Subjects

*RETINAL ganglion cells, *RETINAL injuries, *CASPASES, *WESTERN immunoblotting, *ENZYME-linked immunosorbent assay, *INFLAMMASOMES

Abstract

Background: Retinal ischemia/reperfusion (IR) injury is a common pathological process in many ophthalmic diseases. Interleukin-1β (IL-1β) is an important inflammatory factor involved in the pathology of retinal IR injury, but the mechanism by which IL-1β is regulated in such injury remains unclear. Caspase-11 non-canonical inflammasomes can regulate the synthesis and secretion of IL-1β, but its role in retinal IR injury has not been elucidated. This study aimed to evaluate the role of caspase-11 non-canonical inflammasomes in retinal IR injury. Methods: Retinal IR injury was induced in C57BL/6J mice by increasing the intraocular pressure to 110 mmHg for 60 min. The post-injury changes in retinal morphology and function and in IL-1β expression were compared between caspase-11 gene knockout (caspase-11−/−) mice and wild-type (WT) mice. Morphological and functional changes were evaluated using hematoxylin–eosin staining and retinal whole mount staining and using electroretinography (ERG), respectively. IL-1β expression in the retina was measured using enzyme-linked immunosorbent assay (ELISA). The levels of caspase-11-related protein were measured using western blot analysis. The location of caspase-11 in the retina was determined via immunofluorescence staining. Mouse type I astrocytes C8-D1A cells were used to validate the effects of caspase-11 simulation via hypoxia in vitro. Small-interfering RNA targeting caspase-11 was constructed. Cell viability was evaluated using the MTT assay. IL-1β expression in supernatant and cell lysate was measured using ELISA. The levels of caspase-11-related protein were measured using western blot analysis. Results: Retinal ganglion cell death and retinal edema were more ameliorated, and the ERG b-wave amplitude was better after retinal IR injury in caspase-11−/− mice than in WT mice. Further, caspase-11−/− mice showed lower protein expressions of IL-1β, cleaved caspase-1, and gasdermin D (GSDMD) in the retina after retinal IR injury. Caspase-11 protein was expressed in retinal glial cells, and caspase-11 knockdown played a protective role against hypoxia in C8-D1A cells. The expression levels of IL-1β, cleaved caspase-1, and GSDMD were inhibited after hypoxia in the si-caspase-11 constructed cells. Conclusions: Retinal IR injury activates caspase-11 non-canonical inflammasomes in glial cells of the retina. This results in increased protein levels of GSDMD and IL-1β and leads to damage in the inner layer of the retina. [ABSTRACT FROM AUTHOR]

Published

2024

22. From fat to fire: The lipid–inflammasome connection.

Author

Anand, Paras K.

Subjects

*LIPID metabolism, *NLRP3 protein, *INFLAMMASOMES, *METABOLIC disorders, *FATTY acids, *CELL death

Abstract

Summary Inflammasomes are multiprotein complexes that play a crucial role in regulating immune responses by governing the activation of Caspase‐1, the secretion of pro‐inflammatory cytokines, and the induction of inflammatory cell death, pyroptosis. The inflammasomes are pivotal in effective host defense against a range of pathogens. Yet, overt activation of inflammasome signaling can be detrimental. The most well‐studied NLRP3 inflammasome has the ability to detect a variety of stimuli including pathogen‐associated molecular patterns, environmental irritants, and endogenous stimuli released from dying cells. Additionally, NLRP3 acts as a key sensor of cellular homeostasis and can be activated by disturbances in diverse metabolic pathways. Consequently, NLRP3 is considered a key player linking metabolic dysregulation to numerous inflammatory disorders such as gout, diabetes, and atherosclerosis. Recently, compelling studies have highlighted a connection between lipids and the regulation of NLRP3 inflammasome. Lipids are integral to cellular processes that serve not only in maintaining the structural integrity and subcellular compartmentalization, but also in contributing to physiological equilibrium. Certain lipid species are known to define NLRP3 subcellular localization, therefore directly influencing the site of inflammasome assembly and activation. For instance, phosphatidylinositol 4‐phosphate plays a crucial role in NLRP3 localization to the trans Golgi network. Moreover, new evidence has demonstrated the roles of lipid biosynthesis and trafficking in activation of the NLRP3 inflammasome. This review summarizes and discusses these emerging and varied roles of lipid metabolism in inflammasome activation. A deeper understanding of lipid‐inflammasome interactions may open new avenues for therapeutic interventions to prevent or treat chronic inflammatory and autoimmune conditions. [ABSTRACT FROM AUTHOR]

Published

2024

23. Pseudorabies Virus UL4 protein promotes the ASC-dependent inflammasome activation and pyroptosis to exacerbate inflammation.

Author

Zhang, Xiaohua, Chen, Guiyuan, Yin, Junqing, Nie, Lichen, Li, Linghao, Du, Qian, Tong, Dewen, and Huang, Yong

Subjects

*AUJESZKY'S disease virus, *PYROPTOSIS, *INFLAMMASOMES, *VIRAL proteins, *NLRP3 protein

Abstract

Pseudorabies virus (PRV) infection causes systemic inflammatory responses and inflammatory damages in infected animals, which are associated with the activation of inflammasome and pyroptosis in infected tissues. Here, we identified a critical function of PRV non-structural protein UL4 that enhanced ASC-dependent inflammasome activation to promote pyroptosis. Whereas, the deficiency of viral UL4 was able to reduce ASC-dependent inflammasome activation and the occurrences of pyroptosis. Mechanistically, the 132–145 aa of UL4 permitted its translocation from the nucleus to the cytoplasm to interact with cytoplasmic ASC to promote the activation of NLRP3 and AIM2 inflammasome. Further research showed that UL4 promoted the phosphorylation levels of SYK and JNK to enhance the ASC phosphorylation, which led to the increase of ASC oligomerization, thus promoting the activation of NLRP3 and AIM2 inflammasome and enhanced GSDMD-mediated pyroptosis. In vivo experiments further showed that PRV UL4 (132DVAADAAAEAAAAE145) mutated strain (PRV-UL4mut) infection did not lead to a significant decrease in viral titers at 12 h. p. i, but it induced lower levels of IL-1β, IL-18, and GSDMD-NT, which led to an alleviated inflammatory infiltration and pathological damage in the lungs and brains, and a lower death rate compared with wild-type PRV strain infection. Taken together, our findings unravel that UL4 is an important viral regulator to manipulate the inflammasome signaling and pyroptosis of host cells to promote the pathogenicity of PRV, which might be further exploited as a new target for live attenuated vaccines or therapeutic strategies against pseudorabies in the future. Author summary: The activation of inflammasome and pyroptosis is associated with the rapid death of mice infected with PRV. However, the specific molecular mechanism by which PRV promotes inflammasome overactivation remains elusive. Here, we identified a critical function of PRV non-structural protein UL4 that enhanced ASC-dependent inflammasome activation to promote pyroptosis. Whereas viral UL4 deficiency reduced ASC-dependent inflammasome activation and pyroptosis. Mechanistically, the 132–145 aa of UL4 protein permitted its translocation to interact with ASC in the cytoplasm. During this process, UL4 promoted the phosphorylation levels of JNK and SYK, which enhanced the ASC phosphorylation, leading to increased ASC oligomerization, and ultimately enhanced the ASC-dependent inflammasome activation and subsequent pyropKtosis. In vivo, compared with PRV-WT infection, the PRV UL4 gene (132DVAADAAAEAAAAE145) mutated strain (PRV-UL4mut) not only delayed the death time of pigs and mice but also alleviated the inflammatory infiltration and pathological damage in the lung and brain tissues. Altogether, our findings unravel UL4 as an important regulator of host immune response by manipulating the inflammasome signaling, which may be regarded as a novel live gene-deleted PRV vaccine candidate. [ABSTRACT FROM AUTHOR]

Published

2024

24. The role of inflammasomes as central inflammatory hubs in Mycobacterium tuberculosis infection.

Author

Theobald, Sebastian J., Müller, Tony A., Lange, Dinah, Keck, Katharina, and Rybniker, Jan

Subjects

MYCOBACTERIUM tuberculosis, MYCOBACTERIAL diseases, INFLAMMASOMES, NLRP3 protein, CELL death

Abstract

Mycobacterium tuberculosis (Mtb) infection represents a global health problem and is characterized by formation of granuloma with a necrotic center and a systemic inflammatory response. Inflammasomes have a crucial role in the host immune response towards Mtb. These intracellular multi-protein complexes are assembled in response to pathogen-associated molecular patterns (PAMPs) or danger-associated molecular patterns (DAMPs). Inflammasome platforms activate caspases, leading to the maturation of the proinflammatory cytokines interleukin (IL)-1 and 18 and the cleavage of gasdermin D (GSDMD), a poreforming protein responsible for cytokine release and pyroptotic cell death. Recent in vitro and in vivo findings have highlighted the importance of inflammasome signaling and subsequent necrotic cell death in Mtb-infected innate immune cells. However, we are just beginning to understand how inflammasomes contribute to disease or to a protective immune response in tuberculosis (TB). A detailed molecular understanding of inflammasomeassociated pathomechanisms may foster the development of novel hostdirected therapeutics or vaccines with improved activity. In this mini-review, we discuss the regulatory and molecular aspects of inflammasome activation and the associated immunological consequences for Mtb pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

25. S- acylation of NLRP3 provides a nigericin sensitive gating mechanism that controls access to the Golgi.

Author

Williams, Daniel M. and Peden, Andrew A.

Subjects

*PATTERN perception receptors, *NLRP3 protein, *ACCESS control, *ACYLATION, *INFLAMMASOMES

Abstract

NLRP3 is an inflammasome seeding pattern recognition receptor activated in response to multiple danger signals which perturb intracellular homeostasis. Electrostatic interac- tions between the NLRP3 polybasic (PB) region and negatively charged lipids on the trans-Golgi network (TGN) have been proposed to recruit NLRP3 to the TGN. In this study, we demonstrate that membrane association of NLRP3 is critically dependant on S-acylation of a highly conserved cysteine residue (Cys-130), which traps NLRP3 in a dynamic S-acylation cycle at the Golgi, and a series of hydrophobic residues preceding Cys-130 which act in conjunction with the PB region to facilitate Cys-130 dependent Golgi enrichment. Due to segregation from Golgi localised thio- esterase enzymes caused by a nigericin induced breakdown in Golgi organisation and function, NLRP3 becomes immobilised on the Golgi through reduced de-acylation of its Cys-130 lipid anchor, suggesting that disruptions in Golgi homeostasis are conveyed to NLRP3 through its acylation state. Thus, our work defines a nigericin sensitive S-acylation cycle that gates access of NLRP3 to the Golgi. [ABSTRACT FROM AUTHOR]

Published

2024

26. Purified CDT toxins and a clean deletion within the CDT locus provide novel insights into the contribution of binary toxin in cellular inflammation and Clostridioides difficile infection.

Author

Nabukhotna, Kateryna, Kordus, Shannon L., Shupe, John A., Cano Rodríguez, Rubén, Smith, Anna, Bohannon, Julia K., Washington, M. Kay, and Lacy, D. Borden

Subjects

*CLOSTRIDIOIDES difficile, *DELETION mutation, *INFLAMMASOMES, *DENDRITIC cells, *ANIMAL culture

Abstract

Clostridioides difficile is a spore-forming pathogen and the most common cause of healthcare-associated diarrhea and colitis in the United States. Besides producing the main virulence factors, toxin A (TcdA) and toxin B (TcdB), many of the common clinical strains encode the C. difficile transferase (CDT) binary toxin. The role of CDT in the context of C. difficile infection (CDI) is poorly understood. Inflammation is a hallmark of CDI and multiple mechanisms of inflammasome activation have been reported for TcdA, TcdB, and the organism. Some studies have suggested that CDT contributes to this inflammation through a TLR2-dependent priming mechanism that leads to the suppression of protective eosinophils. Here, we show that CDT does not prime but instead activates the inflammasome in bone marrow-derived dendritic cells (BMDCs). In bone marrow-derived macrophages (BMDMs), the cell binding and pore-forming component of the toxin, CDTb, alone activates the inflammasome and is dependent on K+ efflux. The activation is not observed in the presence of CDTa and is not observed in BMDMs derived from Nlrp3-/- mice suggesting the involvement of the NLRP3 inflammasome. However, we did not observe evidence of CDT-dependent inflammasome priming or activation in vivo. Mice were infected with R20291 and an isogenic CRISPR/Cas9-generated R20291 ΔcdtB strain of C. difficile. While CDT contributes to increased weight loss and cecal edema at 2 days post infection, the relative levels of inflammasome-associated cytokines, IL-1β and IL-18, in the cecum and distal colon are unchanged. We also saw CDT-dependent weightloss in Nlrp3-/- mice, suggesting that the increased weightloss associated with the presence of CDT is not a result of NLRP3-dependent inflammasome activation. This study highlights the importance of studying gene deletions in the context of otherwise fully isogenic strains and the challenge of translating toxin-specific cellular responses into a physiological context, especially when multiple toxins are acting at the same time. Author summary: Clostridioides difficile is a pathogen causing life-threatening diarrhea. C. difficile transferase (CDT) toxin is present in many strains associated with severe disease but its role during C. difficile infection is unclear. In this study, we show that the pore forming subunit, CDTb, activates the inflammasome in myeloid-derived murine cells. While we found that CDT contributes to weight loss in a C. difficile mouse infection model, this was independent of the inflammasome function. This study highlights the importance of studying gene deletions in the context of otherwise fully isogenic strains and the challenge of translating findings in tissue culture models to animal infections. However, it does reveal an additive role for CDT in the tissue edema that occurs in the murine model of acute infection and is consistent with the idea that CDT contributes to the severity of CDI symptoms. [ABSTRACT FROM AUTHOR]

Published

2024

27. Crosstalk between inflammasome sensors and DNA damage response pathways.

Author

Burlet, Delphine, Huber, Anne‐Laure, Tissier, Agnès, and Petrilli, Virginie

Subjects

*DNA repair, *MITOCHONDRIAL DNA, *EUKARYOTIC cells, *INFLAMMASOMES, *NLRP3 protein

Abstract

Eukaryotic cells encounter diverse threats jeopardizing their integrity, prompting the development of defense mechanisms against these stressors. Among these mechanisms, inflammasomes are well‐known for their roles in coordinating the inflammatory response against infections. Extensive research has unveiled their multifaceted involvement in cellular processes beyond inflammation. Recent studies emphasize the intricate relationship between the inflammasome and the DNA damage response (DDR). They highlight how the DDR participates in inflammasome activation and the reciprocal impact of inflammasome on DDR and genome integrity preservation. Moreover, novel functions of inflammasome sensors in DDR pathways have emerged, broadening our understanding of their roles. Finally, this review delves into identifying common signals that drive the activation of inflammasome sensors alongside activation cues for the DNA damage response, offering potential insights into shared regulatory pathways between these critical cellular processes. [ABSTRACT FROM AUTHOR]

Published

2024

28. Enteric glial NLRP3 inflammasome contributes to gut mucosal barrier alterations in a mouse model of diet‐induced obesity.

Author

D'Antongiovanni, Vanessa, Fornai, Matteo, Colucci, Rocchina, Nericcio, Anna, Benvenuti, Laura, Di Salvo, Clelia, Segnani, Cristina, Pierucci, Clarissa, Ippolito, Chiara, Nemeth, Zoltan H., Haskó, György, Bernardini, Nunzia, Antonioli, Luca, and Pellegrini, Carolina

Subjects

*NEUROGLIA, *NLRP3 protein, *BODY weight, *DRUG target, *INFLAMMASOMES

Abstract

Aim Methods Results Conclusion In the present study, we investigated the involvement of NLRP3 inflammasome in the intestinal epithelial barrier (IEB) changes associated with obesity, and its role in the interplay between enteric glia and intestinal epithelial cells (IECs).Wild‐type C57BL/6J and NLRP3‐KO (−/−) mice were fed with high‐fat diet (HFD) or standard diet for 8 weeks. Colonic IEB integrity and inflammasome activation were assessed. Immunolocalization of colonic mucosal GFAP‐ and NLRP3‐positive cells along with in vitro coculture experiments with enteric glial cells (EGCs) and IECs allowed to investigate the potential link between altered IEB, enteric gliosis, and NLRP3 activation.HFD mice showed increased body weight, altered IEB integrity, increased GFAP‐positive glial cells, and NLRP3 inflammasome hyperactivation. HFD‐NLRP3−/− mice showed a lower increase in body weight, an improvement in IEB integrity and an absence of enteric gliosis. Coculture experiments showed that palmitate and lipopolysaccharide contribute to IEB damage and promote enteric gliosis with consequent hyperactivation of enteric glial NLRP3/caspase‐1/IL‐1β signaling. Enteric glial‐derived IL‐1β release exacerbates the IEB alterations. Such an effect was abrogated upon incubation with anakinra (IL‐1β receptor antagonist) and with conditioned medium derived from silenced‐NLRP3 glial cells.HFD intake elicits mucosal enteric gliotic processes characterized by a hyperactivation of NLRP3/caspase‐1/IL‐1β signaling pathway, that contributes to further exacerbate the disruption of intestinal mucosal barrier integrity. However, we cannot rule out the contribution of NLRP3 inflammasome activation from other cells, such as immune cells, in IEB alterations associated with obesity. Overall, our results suggest that enteric glial NLRP3 inflammasome might represent an interesting molecular target for the development of novel pharmacological approaches aimed at managing the enteric inflammation and intestinal mucosal dysfunctions associated with obesity. [ABSTRACT FROM AUTHOR]

Published

2024

29. Characterization of age-associated inflammasome activation reveals tissue specific differences in transcriptional and post-translational inflammatory responses.

Author

Talley, Sarah, Nguyen, Tyler, Van Ye, Lily, Valiauga, Rasa, DeCarlo, Jake, Mustafa, Jabra, Cook, Benjamin, White, Fletcher A., and Campbell, Edward M.

Subjects

*TRANSGENIC mice, *CENTRAL nervous system, *INFLAMMASOMES, *CASPASES, *ENDOTOXINS

Abstract

Aging is associated with systemic chronic, low-grade inflammation, termed 'inflammaging'. This pattern of inflammation is multifactorial and is driven by numerous inflammatory pathways, including the inflammasome. However, most studies to date have examined changes in the transcriptomes that are associated with aging and inflammaging, despite the fact that inflammasome activation is driven by a series of post-translational activation steps, culminating in the cleavage and activation of caspase-1. Here, we utilized transgenic mice expressing a caspase-1 biosensor to examine age-associated inflammasome activation in various organs and tissues to define these post-translational manifestations of inflammaging. Consistent with other studies, we observe increased inflammation, including inflammasome activation, in aged mice and specific tissues. However, we note that the degree of inflammasome activation is not uniformly associated with transcriptional changes commonly used as a surrogate for inflammasome activation in tissues. Furthermore, we used a skull thinning technique to monitor central nervous system inflammasome activation in vivo in aged mice and found that neuroinflammation is significantly amplified in aged mice in response to endotoxin challenge. Together, these data reveal that inflammaging is associated with both transcriptional and post-translational inflammatory pathways that are not uniform between tissues and establish new methodologies for measuring age-associated inflammasome activation in vivo and ex vivo. [ABSTRACT FROM AUTHOR]

Published

2024

30. UK5099 Inhibits the NLRP3 Inflammasome Independently of its Long‐Established Target Mitochondrial Pyruvate Carrier.

Author

Ran, Linyu, Chen, Miao, Ye, Jihui, Zhang, Song, Luo, Zhibing, Bai, Tengfei, Qian, Chenchen, Zhou, Quan, Shan, Mengtian, Chu, Yong, Herrmann, Joerg, Li, Qiang, and Wang, Feilong

Subjects

*NLRP3 protein, *DOUBLE bonds, *DRUG target, *ENDOTOXEMIA, *INFLAMMASOMES

Abstract

Targeting NLRP3 inflammasome has been recognized as a promising therapeutic strategy for the treatment of numerous common diseases. UK5099, a long‐established inhibitor of mitochondrial pyruvate carrier (MPC), is previously found to inhibit macrophage inflammatory responses independent of MPC expression. However, the mechanisms by which UK5099 inhibit inflammatory responses remain unclear. Here, it is shown that UK5099 is a potent inhibitor of the NLRP3 inflammasome in both mouse and human primary macrophages. UK5099 selectively suppresses the activation of the NLRP3 but not the NLRC4 or AIM2 inflammasomes. Of note, UK5099 retains activities on NLRP3 in macrophages devoid of MPC expression, indicating this inhibitory effect is MPC‐independent. Mechanistically, UK5099 abrogates mitochondria‐NLRP3 interaction and in turn inhibits the assembly of the NLRP3 inflammasome. Further, a single dose of UK5099 persistently reduces IL‐1β production in an endotoxemia mouse model. Importantly, structure modification reveals that the inhibitory activities of UK5099 on NLRP3 are unrelated to the existence of the activated double bond within the UK5099 molecule. Thus, this study uncovers a previously unknown molecular target for UK5099, which not only offers a new candidate for the treatment of NLRP3‐driven diseases but also confounds its use as an MPC inhibitor in immunometabolism studies. [ABSTRACT FROM AUTHOR]

Published

2024

31. Inflammatory profile of lower risk myelodysplastic syndromes.

Author

Topping, Joanne, Taylor, Adele, Nadat, Fatima, Crouch, Simon, Ibbotson, Alice, Čermák, Jaroslav, Symeonidis, Argiris, Tatic, Aurelia, Langemeijer, Saskia, Hellström‐Lindberg, Eva, Culligan, Dominic, Garelius, Hege Gravdahl, Ashcroft, John, Nga, Emma, Parker, Jane, Kolade, Seye, McDermott, Michael F., De Witte, Theo, Bowen, David, and Smith, Alexandra

Subjects

*RED blood cell transfusion, *MYELODYSPLASTIC syndromes, *NLRP3 protein, *INFLAMMASOMES, *INTERFERONS

Abstract

Summary: The precise link between inflammation and pathogenesis of myelodysplastic syndrome (MDS) is yet to be fully established. We developed a novel method to measure ASC/NLRP3 protein specks which are specific for the NLRP3 inflammasome only. We combined this with cytokine profiling to characterise various inflammatory markers in a large cohort of patients with lower risk MDS in comparison to healthy controls and patients with defined autoinflammatory disorders (AIDs). The ASC/NLRP3 specks were significantly elevated in MDS patients compared to healthy controls (p < 0.001) and these levels were comparable to those found in patients with AIDs. The distribution of protein specks positive only for ASC was different to ASC/NLRP3 ones suggesting that other ASC‐containing inflammasome complexes might be important in the pathogenesis of MDS. Patients with MDS‐SLD had the lowest levels of interleukin (IL)‐1β, tumour necrosis factor (TNF), IL‐23, IL‐33, interferon (IFN) γ and IFN‐α2, compared to other diagnostic categories. We also found that inflammatory cytokine TNF was positively associated with MDS progression to a more aggressive form of disease and IL‐6 and IL‐1β with time to first red blood cell transfusion. Our study shows that there is value in analysing inflammatory biomarkers in MDS, but their diagnostic and prognostic utility is yet to be fully validated. [ABSTRACT FROM AUTHOR]

Published

2024

32. The NLRP3 inhibitor Dapansutrile improves the therapeutic action of lonafarnib on progeroid mice.

Author

Muela‐Zarzuela, Inés, Suarez‐Rivero, Juan Miguel, Boy‐Ruiz, Daniel, López‐Pérez, Juan, Sotelo‐Montoro, Marta, del Mar Navarrete‐Alonso, Maria, Collado, Isidro G., Botubol‐Ares, José Manuel, Sanz, Alberto, and Cordero, Mario D.

Subjects

*PROGERIN, *HEPATOTOXICOLOGY, *NLRP3 protein, *PROGERIA, *INFLAMMASOMES

Abstract

The role of the inflammasomes in aging and progeroid syndromes remain understudied. Recently, MCC950, a NLRP3 inhibitor, was used in Zmpste24−/− mice to ameliorate the phenotypes. However, the safety of MCC950 was questioned due to liver toxicity observed in humans. Nevertheless, inhibition of the inflammasomes would be a beneficial therapy for progeria. Here, we show that OLT1177 (dapansutrile), other NLRP3 inhibitor, improved cellular and animal phenotypes using progeroid fibroblasts and a LmnaG609G/G609G mouse model. In both cases dapansutrile reduced progerin accumulation, NLRP3‐inflammasome activation and secretory phenotype of senescence, extended the lifespan of progeroid animals, preserved bodyweight, and reduced kyphosis, inflammation, and senescence. Interestingly, dapansutrile further improved the effect of lonafarnib, the only FDA‐approved drug for the progeria. The combination of both drugs reduced the inflammation and senescence, extended survival and ameliorated various progeroid defects both in vitro and in vivo, compared with treatment using lonafarnib alone. These findings and the safety of dapansutrile demonstrated in several clinical trials proposes it as a possible co‐adjuvant treatment with lonafarnid in HGPS. [ABSTRACT FROM AUTHOR]

Published

2024

33. Irisin Prevents Cell Death in High Glucose via NLRP3 Inhibition.

Author

Hanwen Wei, Jing Zhou, Xincheng Qiu, Haiyu Niu, Zheng Zhang, Yanjun Liu, Po Bai, Chao Xin, Wen Wen, Xiaojiong Lu, Guangying Cao, and Taohong Hu

Subjects

*CELL death, *CARDIOVASCULAR diseases, *PROTEIN expression, *INFLAMMASOMES, *AUTOPHAGY, *GLUCOSE

Abstract

Background • Impaired cardiac microvascular function has been implied in the pathophysiology of diabetic cardiovascular disease. However, the specific mechanism remains to be determined. Pyroptosis is a type of cell death that differs from apoptosis and autophagy. It is caused by the formation of plasma membrane pores through aminoterminal fragments of Gasdermin D (GSDMD), leading to the secretion of IL-1β and IL-18. Recent studies have shown that irisin, a myokine cleaved by the extracellular domain of FNDC5, plays a protective role in cardiovascular diseases. Here, we investigated the potential role of pyroptosis on the cardiac microvascular endothelial cells (CMECs) injury induced by high glucose (HG) and further determined the protective effect of irisin on pyroptosis. Methods • CMECs were cultured with normal glucose (control group, 5.5 mM) and high glucose (25 mM) medium for 12, 24, and 48 h respectively. The pyroptosis of CMECs was measured by immunofluorescence staining, ELISA, and Western blot assays. Moreover, the apoptosis level was determined by flow cytometry and TUNEL staining. Results • Our results showed that HG promoted apoptosis and pyroptosis. However, irisin reversed the increased apoptosis and pyroptosis. To investigate the underlying mechanism, we overexpressed the NLRP3 protein. We found the protective effect of irisin on apoptosis and pyroptosis was abolished by NLRP3 over-expression. Conclusions • Our data suggest that irisin protects CMECs against apoptosis and pyroptosis, at least in part, by inhibiting NLRP3 inflammasome. [ABSTRACT FROM AUTHOR]

Published

2024

34. Anoectochilus roxburghii polysaccharide reduces D-GalN/LPS-induced acute liver injury by regulating the activation of multiple inflammasomes.

Author

Yan, Yulu, Ye, Xiqi, Huang, Chunqing, Wu, Junjun, Liu, Yunbiao, Zheng, Pingping, Shen, Congqi, Bai, Zhaofang, and Tingming, Shen

Subjects

*TREATMENT effectiveness, *LIVER enzymes, *POLYSACCHARIDES, *LIVER injuries, *NLRP3 protein

Abstract

Background: Acute liver injury (ALI) is a serious syndrome with a high mortality rate due to viral infection, toxic exposure, and autoimmunity, and its severity can range from mildly elevated liver enzymes to severe liver failure. Activation of the nod-like receptor pyrin domain-containing 3 (NLRP3) inflammasome is closely associated with the development of ALI, and the search for an inhibitor targeting this pathway may be a novel therapeutic option. Anoectochilus roxburghii polysaccharide (ARP) is a biologically active ingredient extracted from Anoectochilus roxburghii with immunomodulatory, antioxidant, and anti-inflammatory bioactivities and pharmacological effects. In this study, we focused on D-galactosamine (D-GalN)/lipopolysaccharide (LPS)-induced acute liver injury by ARP through inhibition of NLRP3 inflammasome. Methods: An inflammasome activation model was established in bone marrow-derived macrophages (BMDMs) to investigate the effects of ARP on caspase-1 cleavage, IL-1β secretion, and ASC oligomerization in inflammasomes under different agonists. We used the D-GalN/LPS-induced acute liver injury model in mice, intraperitoneally injected ARP or MCC950, and collected liver tissues, serum, and intraperitoneal lavage fluid for pathological and biochemical indexes. Results: ARP effectively inhibited the activation of the NLRP3 inflammasome and had an inhibitory effect on non-classical NLRP3, AIM2, and NLRC4 inflammasomes. It also effectively inhibited the oligomerization of apoptosis-associated speck-like protein (ASC) from a variety of inflammatory vesicles. Meanwhile, ARP has good therapeutic effects on acute liver injury induced by D-GaIN/LPS. Conclusion: The inhibitory effect of ARP on a wide range of inflammasomes, as well as its excellent protection against acute liver injury, suggests that ARP may be a candidate for acute liver injury. [ABSTRACT FROM AUTHOR]

Published

2024

35. Future Therapeutics: Targeting the NLRP3 Inflammasome Pathway to Manage Diabetic Retinopathy Development and Progression.

Author

Kuo, Charisse Y. J., Rupenthal, Ilva D., Murphy, Rinki, and Mugisho, Odunayo O.

Subjects

*NLRP3 protein, *VISION disorders, *INFLAMMASOMES, *DISEASE progression, *FENOFIBRATE, *DIABETIC retinopathy

Abstract

While existing local therapies partially restore vision loss from diabetic retinopathy (DR), there is currently no reliable treatment to prevent the onset or stop the progression of the disease. This review seeks to explore the inflammatory molecular mechanisms underpinning DR pathogenesis, which have not been targeted by current interventions. Specifically, this review explores the role of the nucleotide-binding oligomerization domain (NOD)-like receptor (NLR) protein 3 (NLRP3) inflammasome in DR onset and progression. Evidence through clinical trials has begun to note that specific drugs (fenofibrate, metformin) appear effective in slowing DR progression independent of lipid or glucose-lowering, respectively, suggesting that other mechanisms are at play. Novel therapeutics that inhibit the activation of the NLRP3 inflammasome pathway may provide a novel treatment for halting DR progression. [ABSTRACT FROM AUTHOR]

Published

2024

36. Endoplasmic Reticulum Stress Signaling in the Regulation of Hepatic Pathological Responses.

Author

Baral, Ananda

Subjects

*ENDOPLASMIC reticulum, *INTRACELLULAR calcium, *CELL death, *INFLAMMASOMES, *INTERLEUKIN-1

Abstract

The endoplasmic reticulum (ER) is a vital cell organelle that is primarily involved in the processes of protein folding, maintenance of intracellular calcium storage and lipid synthesis in order to maintain cellular homeostasis. To achieve this meticulous order, several ER-dependent processes have to be in unison and perfect harmony. However, a persistent supply of newly synthesized proteins strains the ER mainly due to the accumulation of unfolded proteins, thus ultimately leading to an imbalance termed ER stress. Although the accumulation of misfolded proteins is a frequent reason for the initiation of ER stress, it is also induced by the hyper-production of reactive oxygen species, aberrant calcium leakage from the ER and due to the effect of cytokines. ER stress signals are conveyed via three arms of ER, namely PERK, IRE1 and ATF6. Signal transduction form these signaling molecules often converges on the transcriptional upregulation of CHOP and its related signaling mechanisms. If the ER stress is unresolved, then it can lead to cell death through different cell death mechanisms, including apoptosis, proptosis, etc. In the liver, it has been observed that ER stress plays a critical role in hepatic damage under different experimental conditions. This review highlights the role of ER stress in liver pathologies. [ABSTRACT FROM AUTHOR]

Published

2024

37. 法舒地尔通过抑制 NLRP3 炎症小体激活抑制 Aβ1-42 诱导的小胶质细胞炎症 反应.

Author

郭敏芳, 章培军, 于婧文, 孟 涛, 李艳花, 李 娜, 李梦迪, 李玉璐, 宋丽娟, 尉杰忠, and 马存根

Subjects

*NLRP3 protein, *CELL morphology, *CASPASES, *INFLAMMASOMES, *WESTERN immunoblotting

Abstract

Objective: To explore mechanism of Fasudil reducing Aβ1-42 induced BV2 cell injury based on NLRP3 inflamma‑ some. Methods: BV2 cells were divided into: normal control group, Aβ stimulation group, Aβ +Fasudil intervention group, Aβ + MCC950 (NLRP3 inhibitor) intervention group. Cell morphology was observed under microscope. Cell activity was determined of by CCK8. NO release was measured by Griess. NLRP3, caspase 1 and IL-18 expressions were detected by immunofluorescence staining. NLRP3, ASC, caspase 1, IL-1β and IL-18 expressions were detected by Western blot. Results: Compared with normal control group, BV2 cells in Aβ stimulation group were activated and showed amoeba-like shape, cell activity was decreased, NO production was increased, NLRP3, ASC, caspase 1, IL-1β and IL-18 expressions were increased. Fasudil intervention and MCC950 intervention inhibited cell injury induced by Aβ1-42 in which BV2 cell morphology tended to be normal, cell activity was increased, while produc‑ tion of NO was reduced, and NLRP3, ASC, caspase 1, IL-1β and IL-18 expressions were down-regulated, there was no significant difference between Fasudil intervention group and MCC950 intervention group. Conclusion: Fasudil may alleviate Aβ1-42 induced BV2 cell injury and inflammatory reaction by inhibiting NLRP3 inflammasome activation. [ABSTRACT FROM AUTHOR]

Published

2024

38. Does NLRP1 Inflammasome Activation in Immune Cells in Kidney Transplantation Relate with Donor Organ Age?

Author

Suarez-Rivero, Juan Miguel, López-Pérez, Juan, Astorga-Gamaza, Antonio, Muela-Zarzuela, Inés, de la Varga-Martínez, Raquel, Aguilera, Aurora, Garcia, Teresa, Mazuecos, Auxiliadora, and Cordero, Mario D.

Subjects

*KIDNEY transplantation, *CELL transplantation, *OLDER patients, *INFLAMMASOMES, *PROTEIN expression, *DEAD, *BRAIN death

Abstract

Inflammation causes a wide range of health disorders. In this process, the formation of inflammasome complexes plays a key role. Although inflammasomes have been extensively studied during kidney disease, their role in kidney transplantation has not been fully elucidated. In this study, we evaluate the gene and protein expression of several components of the inflammasome pathway before and at several time points after kidney transplantation in a cohort of patients of different ages and receiving an organ from older or younger donors. Our findings indicate the activation of the NLRP1 inflammasome in several immune cell population, monocytes and CD4+ and CD8+ cells mainly, in renal transplant, and its level increases gradually in patients who receive an older organ, whereas it has the opposite effect on older patients who receive a younger organ. Despite treatment with immunosuppressants, inflammation persists in some patients. These results lead to the hypothesis that the donor's age is a critical factor in post-transplant inflammasome activation and that specific NLRP1 inflammasome inhibitors should be considered to increase the success of kidney transplantation long-term.  Color images are available online. [ABSTRACT FROM AUTHOR]

Published

2024

39. Hydroxychloroquine as an Adjunct Therapy for Diabetes in Pregnancy.

Author

Basri, Nurul Iftida, Murthi, Padma, and Abd Rahman, Rahana

Subjects

*GESTATIONAL diabetes, *PREGNANCY outcomes, *HYDROXYCHLOROQUINE, *OXIDATIVE stress, *INFLAMMASOMES

Abstract

This review discusses the pathophysiology of diabetes in pregnancy in relation to the placental function. We review the potential use of hydroxychloroquine in improving pregnancy outcomes affected by diabetes. The review focuses on the mechanism of action of hydroxychloroquine and its potential effects on diabetes. There are several pathways in which hydroxychloroquine mediates its effects: through the inflammasome complex, inflammatory cytokines, oxidative stress, modulatory effects, and antihyperglycemic effects. As a safe drug to be used in pregnancy, it is worth exploring the possible use hydroxychloroquine as an adjunct treatment to the current therapy of diabetes in pregnancy. [ABSTRACT FROM AUTHOR]

Published

2024

40. The long non-coding RNA mir155hg promotes NLRP3-inflammasome activation and oxidative stress response in acute lung injury by targeting miR-450b-5p to regulate HIF-1α.

Author

Wang, Gui Na, Yang, Miao, Wu, Bo, Huo, Yan, and Xu, Wei

Subjects

*FLUORESCENCE in situ hybridization, *LINCRNA, *ENZYME-linked immunosorbent assay, *INFLAMMASOMES, *NLRP3 protein, *NON-coding RNA

Abstract

Acute lung injury (ALI) can cause multiple organ dysfunction and a high mortality rate. Inflammatory responses, oxidative stress, and immune damage contribute to their pathogenic mechanisms. We studied the role of the newly discovered lncRNA, Lncmir155hg, in ALI. The levels of Lncmir155hg and miR-450b-5p from mice with ALI were detected via polymerase chain reaction analysis (qRT-PCR) and Fluorescence in situ hybridization (FISH). Pathological changes of lung were detected by HE (hematoxylin and eosin) staining, and HIF-1α, NOD-like receptor 3 (NLRP3) and caspase-1 protein changes were detected by immunohistochemistry. MLE-12 cells proliferation was detected by Cell-Counting Kit 8 analysis, and reactive oxygen species (ROS) was detected via flow cytometry. NLRP3, apoptosis-associated speck-like protein (ASC), and caspase-1 were measured via western blotting, and enzyme-linked immunosorbent assays detected the expression of Inflammatory factors. Lncmir155hg, miR-450b-5p, miR-450b-5p, and HIF-1α targets were predicted using LncTar and miRWalk and confirmed in dual-luciferase reporter assays. In mice with ALI and MLE-12 cells induced by lipopolysaccharide (LPS), Lncmir155hg was high-expressed and miR-450b-5p was low-expressed. sh-Lncmir155hg reduced the damage of lung tissue, the production of inflammatory cytokines and oxidative stress reaction induced by LPS，miR-450b-5p reverses the effect of Lncmir155hg in mice. sh-Lncmir155hg decreased the protein levels of HIF-1α, NLRP3 and caspase-1 in LPS-induced lung tissues. sh-Lncmir155hg + miR-450b-5p inhibitor transfection reversed the effect of sh-Lncmir155hg on the expression of HIF-1α, NLRP3 and caspase-1. Lncmir155hg knockdown induced proliferation and inhibited NLRP3-inflammasome activation and oxidative stress in MLE-12 cells of ALI. miR-450b-5p was identified to have binding with Lncmir155hg, and inhibition of miR-450b-5p eliminated the effect of si-Lncmir155hg in MLE-12 cells of ALI. More importantly, miR-450b-5p was directly combined with HIF-1α, miR-450b-5p mimic promoted proliferation and inhibited activation of inflammasome associated proteins and reaction of oxidative stress, and HIF-1α overexpression abolished these effects. Lncmir155hg aggravated ALI via the miR-450b-5p/HIF-1α axis. In this study, ALI mouse model was prepared by intratracheal injection of LPS. Whole transcriptome sequencing was performed on normal and ALI mice. Through bioinformatics analysis, we found that Lncmir155hg was upregulated in the lung tissue of ALI mice. The upregulation of Lncmir155hg suppressed miR-450b-5p, which further enhanced the expression of HIF-1α, regulating the proliferation of alveolar epithelial cells and regulating NLRP3 inflammasome and oxidative-stress responses of alveolar epithelium and lung tissue, ultimately leading to ALI. [Display omitted] • lncmir155hg promotes NLRP3-inflammasome activation and oxidative stress response in ALI. • lncmir155hg promotes ALI progression by sponging miR-450b-5p. • miR-450b-5p targeted HIF-1α to inhibit lncmir155hg-mediated ALI progression. [ABSTRACT FROM AUTHOR]

Published

2024

41. Heparan sulfate acts as an activator of the NLRP3 inflammasome promoting inflammatory response in the development of acute pancreatitis.

Author

Zhao, Li-Jun, Chen, Peng, Huang, Ling, He, Wen-Qi, Tang, Ying-Rui, Wang, Rui, Luo, Zhu-Lin, and Ren, Jian-Dong

Subjects

*HEPARAN sulfate, *NLRP3 protein, *PROTEIN receptors, *INFLAMMASOMES, *HEPARANASE

Abstract

Background: Accumulating evidence has shown that the NOD-like receptor protein 3 (NLRP3) inflammasome plays a crucial role in the inflammatory cascades involved in the development of acute pancreatitis (AP). However, the specific agonist responsible for activating the NLRP3 inflammasome in this process has not yet been identified. The purpose of this study is to clarify whether heparan sulfate (HS) works as an NLRP3 inflammasome activator to evoke inflammatory cascades in the progression of AP. Methods: Two experimental mouse models of AP were utilized to investigate the pro-inflammatory activity of HS in the development of AP by measuring the secretion of inflammatory cytokines and the neutrophil infiltration in pancreatic tissue. The ability of HS to activate the NLRP3 inflammasome was evaluated both in vitro and in vivo. The nuclear factor kappa B (NF-κB)-mediated expression of NLRP3 inflammasome components in response to HS treatment was determined to decipher the role of HS in transcriptional priming of NLRP3 inflammasome. Furthermore, HS-triggered deubiquitination of NLRP3 was analyzed to reveal the promoting effect of HS on the NLRP3 inflammasome priming via a non-transcriptional pathway. Results: High plasma level of HS was observed with a positive correlation to that of inflammatory cytokines in AP mice. Administration of HS to mice resulted in an exacerbated inflammatory profile, while reducing HS production by an inhibitor of heparanase significantly attenuated inflammatory response. Pharmacological inhibition or genetic deletion of NLRP3 substantially suppressed the HS-stimulated elevation of IL-1β levels in AP mice. The in vitro data demonstrated that HS primarily serves as a priming signal for the activation of the NLRP3 inflammasome. HS possesses the ability to increase the transcriptional activity of NF-κB and TLR4/NF-κB-driven transcriptional pathway is employed for NLRP3 inflammasome priming. Moreover, HS-induced deubiquitination of NLRP3 is another pathway responsible for non-transcriptional priming of NLRP3 inflammasome. Conclusions: Our current work has unveiled HS as a new activator of the NLRP3 inflammasome responsible for the secondary inflammatory cascades during the development of AP, highlighting the HS-NLRP3 pathway as a potential target for future preventive and therapeutic approaches of AP. [ABSTRACT FROM AUTHOR]

Published

2024

42. Tanshinone I limits inflammasome activation of macrophage via docking into Syk to alleviate DSS-induced colitis in mice.

Author

Hu, Chunmiao, He, Xiaoli, Zhang, Huimin, Hu, Xiangyu, Liao, Liting, Cai, Minmin, Lin, Zhijie, Xiang, Jie, Jia, Xiaoqin, Lu, Guotao, Xiao, Weiming, Feng, Yisheng, and Gong, Weijuan

Subjects

*SURFACE plasmon resonance, *MACROPHAGE activation, *INTRAPERITONEAL injections, *COLITIS, *INFLAMMASOMES

Abstract

Tanshinone I (Tan I) has been proven to exert an anti-inflammatory effect, but the complete mechanism remains unclear. In this study, Tan I was described to have no effect on Syk expression in resting or LPS-stimulated macrophages ex vivo , but dramatically suppressed Syk phosphorylation and CD80, CD86, and IL-1β expression of macrophages. The inflammatory activity of macrophages in ApoC3-transgenic (ApoC3TG) mice is upregulated by Syk activation. Tan I was determined to downregulate Syk phosphorylation and inflammatory activity of macrophages in ApoC3TG mice, both ex vivo and in vivo. Intraperitoneal injection of Tan I (4 mg/kg) effectively alleviated DSS-induced colitis in mice, accompanying with suppressing the activation of intestinal macrophages. Mechanistically, Tan I-treated macrophages exhibited a decrease in cytoplasmic ROS, NLRP3, GSDMD, and IL-1β, which suggested that the alternative pathway of inflammasome activation in macrophages was suppressed. The SPR assay demonstrated that Tan I bound to Syk protein with a dissociation constant (KD) of 2.473 × 10−6 M. When Syk expression was knocked down by its shRNA, the inhibitory effects of Tan I on macrophages were blocked. Collectively, Tanshinone I effectively alleviated DSS-induced colitis in mice by inhibiting Syk-stimulated inflammasome activation, hence suppressing the inflammatory activity of macrophages. • Tanshinone I inhibited p-Syk and limited the inflammatory activity of macrophages. • Tanshinone I effectively alleviated DSS-induced colitis in mice by limiting the activation of intestinal macrophages. • Tanshinone I-treated macrophages exhibited a decrease in alternative pathway of inflammasome activation. • Direct binding of Tanshinone Ⅰ to Syk was confirmed by the surface plasmon resonance assay. [ABSTRACT FROM AUTHOR]

Published

2024

43. NLRP3 Inflammasome Inhibition After Pilocarpine-Induced Status Epilepticus Attenuates Chronic Inflammation in Epileptic Mice.

Author

Wang, Lei, Wang, Kai, Chen, Yuwen, Zhang, Xiaoyu, Xu, Wenhao, Dong, Zhong, and Wang, Yu

Subjects

ENZYME-linked immunosorbent assay, STATUS epilepticus, NLRP3 protein, POLYMERASE chain reaction, INFLAMMASOMES

Abstract

To investigate the effects of inhibiting the NOD-like receptor family pyrin domain-containing 3 (NLRP3) inflammasome on neuronal damage and chronic pro-inflammatory responses during epileptogenesis in a mouse model of pilocarpine-induced status epilepticus (SE). Methods: Mice were randomly allocated into three groups: control, SE, and SE + MCC 950. The expression patterns of M1 and M2 microglial biomarkers in the hippocampus were quantified using Western blotting, quantitative real-time polymerase chain reaction, enzyme-linked immunosorbent assay, and immunofluorescence staining. Additionally, seizure susceptibility, video-electroencephalography recording, Morris water maze test, and brain immunofluorescence staining were performed to evaluate the epileptic brain 4 weeks post-SE. Results: Within 72 hours post-SE, hippocampal microglia demonstrated a preferential polarization towards the M1 phenotype, a trend that was mitigated by NLRP3 inflammasome inhibition. During epileptogenesis, SE mice treated with NLRP3 inflammasome inhibition exhibited reduced neuronal damage, improved cognitive function, decreased seizure susceptibility, and attenuated chronic pro-inflammatory responses. Conclusion: Inhibition of NLRP3 inflammasome post-SE effectively ameliorates neuronal loss, seizure susceptibility, and cognitive dysfunction during epileptogenesis. This neuroprotective effect may be mediated through the mitigation of chronic pro-inflammatory responses within the epileptic brain. [ABSTRACT FROM AUTHOR]

Published

2024

44. Host microbiome associated low intestinal acetate correlates with progressive NLRP3-dependent hepatic-immunotoxicity in early life microcystin-LR exposure.

Author

Bose, Dipro, Trivedi, Ayushi, Roy, Subhajit, Chatterjee, Saurabh, More, Madhura, Chatterjee, Somdatta, and Saha, Punnag

Subjects

Acetate, GPR43, Microbiome, Microcystin, NLRP3, Animals, Mice, Acetates, Dysbiosis, Gastrointestinal Microbiome, Inflammasomes, Inflammation, Microcystins, NLR Family, Pyrin Domain-Containing 3 Protein

Abstract

BACKGROUND: Microcystins (MCs), potent hepatotoxins pose a significant health risk to humans, particularly children, who are more vulnerable due to higher water intake and increased exposure during recreational activities. METHODS: Here, we investigated the role of host microbiome-linked acetate in modulating inflammation caused by early-life exposure to the cyanotoxin Microcystin-LR (MC-LR) in a juvenile mice model. RESULTS: Our study revealed that early-life MC-LR exposure disrupted the gut microbiome, leading to a depletion of key acetate-producing bacteria and decreased luminal acetate concentration. Consequently, the dysbiosis hindered the establishment of a gut homeostatic microenvironment and disrupted gut barrier function. The NOD-like receptor family pyrin domain - containing 3 (NLRP3) inflammasome, a key player in MC-induced hepatoxicity emerged as a central player in this process, with acetate supplementation effectively preventing NLRP3 inflammasome activation, attenuating hepatic inflammation, and decreasing pro-inflammatory cytokine production. To elucidate the mechanism underlying the association between early-life MC-LR exposure and the progression of metabolic dysfunction associated steatotic liver disease (MASLD), we investigated the role of acetate binding to its receptor -G-protein coupled receptor 43 (GPR43) on NLRP3 inflammasome activation. Our results demonstrated that acetate-GPR43 signaling was crucial for decreasing NLRP3 protein levels and inhibiting NLRP3 inflammasome assembly. Further, acetate-induced decrease in NLRP3 protein levels was likely mediated through proteasomal degradation rather than autophagy. Overall, our findings underscore the significance of a healthy gut microbiome and its metabolites, particularly acetate, in the progression of hepatotoxicity induced by early life toxin exposure, crucial for MASLD progression. CONCLUSIONS: This study highlights potential therapeutic targets in gut dysbiosis and NLRP3 inflammasome activation for mitigating toxin-associated inflammatory liver diseases.

Published

2023

45. CARD8 polymorphisms among bacterial meningitis patients in North-West Ethiopia

Author

Meseret Belayneh, Mesfin Mengesha, Berhane A. Idosa, Surafel Fentaw, Biniyam Moges, Zelalem Tazu, Meseret Assefa, Örjan Garpenholt, Alexander Persson, Eva Särndahl, Ebba Abate, Olof Säll, and Baye Gelaw

Subjects

Meningitis, Inflammasomes, CARD 8 polymorphisms, Neisseria meningitidis, Streptococcus pneumoniae, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background The severity of infectious disease outcomes is dependent on the virulence factors of the pathogen and the host immune response. CARD8 is a major regulator of the innate immune proinflammatory response and has been suggested to modulate the host response to common inflammatory diseases. In the present study, the C10X genetic polymorphism in the CARD8 gene was investigated in relation to bacterial meningitis. Methods A total of 400 clinically suspected meningitis patients hospitalized at the University of Gondar Hospital were enrolled in the study. Cerebrospinal fluid (CSF) and blood samples were collected for laboratory investigations. The collected CSF was cultured, and all the results obtained from the culture were confirmed using direct RT‒PCR. Genotyping of whole-blood samples was performed using a TaqMan assay. The results were compared with apparently healthy controls and with PCR-negative meningitis suspected patients. Results Of the included patients, 57% were men and the most common clinical signs and symptoms were fever (81%), headache (80%), neck stiffness (76%), nausea (68%), and vomiting (67%). Microbiology culture identified 7 patients with bacterial meningitis caused by Neisseria meningitidis (n = 4) and Streptococcus pneumoniae (n = 3). The RT-PCR revealed 39 positive samples for N. meningitidis (n = 10) and S. pneumoniae (n = 29). A total of 332 whole-blood samples were genotyped with the following results: 151 (45.5%) C10X heterozygotes, 59 (17.7%) C10X homozygotes and 122 (36.7%) wild genotypes. The polymorphic gene carriers among laboratory confirmed, clinically diagnosed meningitis and healthy controls were 23(46%), 246(40%), and 1526(39%), respectively with OR = 1.27 (0.7–2.3) and OR = 1.34 (0.76–2.4). The presence of the C10X polymorphism in the CARD8 gene was more prevalent in suspected meningitis patients than in healthy controls (OR 1.2; 1.00-1.5). Homozygote C10X polymorphic gene carriers were more susceptible to infectious disease. The presence of viable or active bacterial infection was found to be associated with the presence of heterozygous C10X carriers. Conclusions A greater proportion of C10X in the CARD8 gene in confirmed bacterial meningitis patients and clinically diagnosed meningitis patients than in healthy controls. Homozygote C10X polymorphic gene carriers were more susceptible to infectious disease than heterozygote gene carriers and healthy controls.

Published

2024

46. Gasdermin D is the only Gasdermin that provides protection against acute Salmonella gut infection in mice.

Author

Maurer, Luca, Geiser, Petra, Bernard, Elliott, Enz, Ursina, Ganguillet, Suwannee, Gül, Ersin, Kroon, Sanne, Demarco, Benjamin, Mack, Vanessa, Furter, Markus, Barthel, Manja, Pelczar, Pawel, Shao, Feng, Broz, Petr, Sellin, Mikael, Hardt, Wolf-Dietrich, and Fattinger, Stefan

Subjects

immunology, microbiology, pathogen, pyroptosis, Animals, Mice, Gasdermins, Salmonella Infections, Salmonella typhimurium, Inflammation, Epithelial Cells, Inflammasomes

Abstract

Gasdermins (GSDMs) share a common functional domain structure and are best known for their capacity to form membrane pores. These pores are hallmarks of a specific form of cell death called pyroptosis and mediate the secretion of pro-inflammatory cytokines such as interleukin 1β (IL1β) and interleukin 18 (IL18). Thereby, Gasdermins have been implicated in various immune responses against cancer and infectious diseases such as acute Salmonella Typhimurium (S.Tm) gut infection. However, to date, we lack a comprehensive functional assessment of the different Gasdermins (GSDMA-E) during S.Tm infection in vivo. Here, we used epithelium-specific ablation, bone marrow chimeras, and mouse lines lacking individual Gasdermins, combinations of Gasdermins or even all Gasdermins (GSDMA1-3C1-4DE) at once and performed littermate-controlled oral S.Tm infections in streptomycin-pretreated mice to investigate the impact of all murine Gasdermins. While GSDMA, C, and E appear dispensable, we show that GSDMD i) restricts S.Tm loads in the gut tissue and systemic organs, ii) controls gut inflammation kinetics, and iii) prevents epithelium disruption by 72 h of the infection. Full protection requires GSDMD expression by both bone-marrow-derived lamina propria cells and intestinal epithelial cells (IECs). In vivo experiments as well as 3D-, 2D-, and chimeric enteroid infections further show that infected IEC extrusion proceeds also without GSDMD, but that GSDMD controls the permeabilization and morphology of the extruding IECs, affects extrusion kinetics, and promotes overall mucosal barrier capacity. As such, this work identifies a unique multipronged role of GSDMD among the Gasdermins for mucosal tissue defense against a common enteric pathogen.

Published

2023

47. Intracellular replication of Pseudomonas aeruginosa in epithelial cells requires suppression of the caspase-4 inflammasome.

Author

Kroken, Abby, Klein, Keith, Mitchell, Patrick, Nieto, Vincent, Jedel, Eric, Evans, David, and Fleiszig, Suzanne

Subjects

Pseudomonas aeruginosa, caspase-4, cornea, epithelium, inflammasome, keratitis, pyroptosis, type three secretion system, Humans, HeLa Cells, Pseudomonas aeruginosa, Inflammasomes, Epithelial Cells, Vacuoles

Abstract

Pathogenesis of Pseudomonas aeruginosa infections can include bacterial survival inside epithelial cells. Previously, we showed that this involves multiple roles played by the type three secretion system (T3SS), and specifically the effector ExoS. This includes ExoS-dependent inhibition of a lytic host cell response that subsequently enables intracellular replication. Here, we studied the underlying cell death response to intracellular P. aeruginosa, comparing wild-type to T3SS mutants varying in capacity to induce cell death and that localize to different intracellular compartments. Results showed that corneal epithelial cell death induced by intracellular P. aeruginosa lacking the T3SS, which remains in vacuoles, correlated with the activation of nuclear factor-κB as measured by p65 relocalization and tumor necrosis factor alpha transcription and secretion. Deletion of caspase-4 through CRISPR-Cas9 mutagenesis delayed cell death caused by these intracellular T3SS mutants. Caspase-4 deletion also countered more rapid cell death caused by T3SS effector-null mutants still expressing the T3SS apparatus that traffic to the host cell cytoplasm, and in doing so rescued intracellular replication normally dependent on ExoS. While HeLa cells lacked a lytic death response to T3SS mutants, it was found to be enabled by interferon gamma treatment. Together, these results show that epithelial cells can activate the noncanonical inflammasome pathway to limit proliferation of intracellular P. aeruginosa, not fully dependent on bacterially driven vacuole escape. Since ExoS inhibits the lytic response, the data implicate targeting of caspase-4, an intracellular pattern recognition receptor, as another contributor to the role of ExoS in the intracellular lifestyle of P. aeruginosa. IMPORTANCE Pseudomonas aeruginosa can exhibit an intracellular lifestyle within epithelial cells in vivo and in vitro. The type three secretion system (T3SS) effector ExoS contributes via multiple mechanisms, including extending the life of invaded host cells. Here, we aimed to understand the underlying cell death inhibited by ExoS when P. aeruginosa is intracellular. Results showed that intracellular P. aeruginosa lacking T3SS effectors could elicit rapid cell lysis via the noncanonical inflammasome pathway. Caspase-4 contributed to cell lysis even when the intracellular bacteria lacked the entire T33S and were consequently unable to escape vacuoles, representing a naturally occurring subpopulation during wild-type infection. Together, the data show the caspase-4 inflammasome as an epithelial cell defense against intracellular P. aeruginosa, and implicate its targeting as another mechanism by which ExoS preserves the host cell replicative niche.

Published

2023

48. Genetic modification of inflammation- and clonal hematopoiesis-associated cardiovascular risk.

Author

Yu, Zhi, Fidler, Trevor, Ruan, Yunfeng, Vlasschaert, Caitlyn, Nakao, Tetsushi, Uddin, Md, Mack, Taralynn, Niroula, Abhishek, Heimlich, J, Zekavat, Seyedeh, Gibson, Christopher, Griffin, Gabriel, Wang, Yuxuan, Peloso, Gina, Heard-Costa, Nancy, Levy, Daniel, Vasan, Ramachandran, Aguet, François, Ardlie, Kristin, Taylor, Kent, Rich, Stephen, Libby, Peter, Jaiswal, Siddhartha, Ebert, Benjamin, Bick, Alexander, Tall, Alan, Natarajan, Pradeep, and Rotter, Jerome

Subjects

Cardiology, Cardiovascular disease, Genetics, Mouse models, Population genetics, Humans, Animals, Mice, Cardiovascular Diseases, Clonal Hematopoiesis, Risk Factors, Inflammasomes, Hematopoiesis, Inflammation, Heart Disease Risk Factors, Mutation

Abstract

Clonal hematopoiesis of indeterminate potential (CHIP) is associated with an increased risk of cardiovascular diseases (CVDs), putatively via inflammasome activation. We pursued an inflammatory gene modifier scan for CHIP-associated CVD risk among 424,651 UK Biobank participants. We identified CHIP using whole-exome sequencing data of blood DNA and modeled as a composite, considering all driver genes together, as well as separately for common drivers (DNMT3A, TET2, ASXL1, and JAK2). We developed predicted gene expression scores for 26 inflammasome-related genes and assessed how they modify CHIP-associated CVD risk. We identified IL1RAP as a potential key molecule for CHIP-associated CVD risk across genes and increased AIM2 gene expression leading to heightened JAK2- and ASXL1-associated CVD risk. We show that CRISPR-induced Asxl1-mutated murine macrophages had a particularly heightened inflammatory response to AIM2 agonism, associated with an increased DNA damage response, as well as increased IL-10 secretion, mirroring a CVD-protective effect of IL10 expression in ASXL1 CHIP. Our study supports the role of inflammasomes in CHIP-associated CVD and provides evidence to support gene-specific strategies to address CHIP-associated CVD risk.

Published

2023

49. Bushen Huoxue formula protects against renal fibrosis and pyroptosis in chronic kidney disease by inhibiting ROS/NLRP3-mediated inflammasome activation.

Author

Liao, Lin, Tao, Pengyu, Xu, Qiming, Chen, Jie, Liu, Weiwei, Hu, Jing, and Lu, Jianrao

Subjects

*RENAL fibrosis, *ANGIOTENSIN II, *CHRONIC kidney failure, *PYROPTOSIS, *INFLAMMASOMES, *STAINS & staining (Microscopy)

Abstract

Renal fibrosis contributes to chronic renal failure and a decline in the quality of life. Bushen Huoxue (BSHX) formula is a Traditional Chinese Medicine used to treat chronic renal failure. However, its mechanisms of action remain unclear. In this study, a rat model of renal fibrosis was constructed by 5/6 nephrectomy in vivo, and histopathological changes were analyzed using hematoxylin-eosin and Masson's trichrome staining. Angiotensin II (Ang II) was used to establish an in vitro renal fibrosis cell model in vitro. Pyroptosis was measured using flow cytometry. Related markers of fibrosis and NOD-like receptor protein 3 (NLRP3) inflammasome activation were measured using western blotting and enzyme-linked immunosorbent assay. Treatment with BSHX (0.25, 0.5, and 1 g/kg) significantly inhibited renal fibrosis and damage in 5/6 nephrectomized rats and simultaneously reduced oxidative stress and NLRP3 inflammasome activation. Similarly, BSHX treatment reduced the levels of hydroxyproline, transforming growth factor-β, matrix metalloproteinase 2, and matrix metalloproteinase 9 and inactivated the Smad2/3 signaling pathway in Ang II-treated HK-2 cells. Our data also showed that treatment with BSHX reduced NLRP3 inflammasome activation and pyroptosis in Ang II-treated HK-2 cells. Moreover, fibrosis and pyroptosis in HK-2 cells induced by NLRP3 overexpression were reduced by treatment with BSHX. BSHX significantly reduced renal fibrosis and pyroptosis, and its mechanism was mainly associated with the inhibition of reactive oxygen species (ROS)/NLRP3-mediated inflammasome activation. [ABSTRACT FROM AUTHOR]

Published

2024

50. The role of NLRP3 inflammasome in type 2 inflammation related diseases.

Author

Shenming Xu, Dan Wang, Lina Tan, and Jianyun Lu

Subjects

*NLRP3 protein, *INFLAMMASOMES, *INFLAMMATION, *ION channels, *ALLERGIC rhinitis

Abstract

Type 2 inflammation related diseases, such as atopic dermatitis, asthma, and allergic rhinitis, are diverse and affect multiple systems in the human body. It is common for individuals to have multiple co-existing type 2 inflammation related diseases, which can impose a significant financial and living burden on patients. However, the exact pathogenesis of these diseases is still unclear. The NLRP3 inflammasome is a protein complex composed of the NLRP3 protein, ASC, and Caspase-1, and is activated through various mechanisms, including the NF-κB pathway, ion channels, and lysosomal damage. The NLRP3 inflammasome plays a role in the immune response to pathogens and cellular damage. Recent studies have indicated a strong correlation between the abnormal activation of NLRP3 inflammasome and the onset of type 2 inflammation. Additionally, it has been demonstrated that suppressing NLRP3 expression effectively diminishes the inflammatory response, highlighting its promising therapeutic applications. Therefore, this article reviews the role of NLRP3 inflammasome in the development and therapy of multiple type 2 inflammation related diseases. [ABSTRACT FROM AUTHOR]

Published

2024