Caspase-11 Mediates Neutrophil Chemotaxis and Extracellular Trap Formation During Acute Gouty Arthritis Through Alteration of Cofilin Phosphorylation

Caution, Kyle; Young, Murray; Robledo‐Avila, Frank; Krause, Kathrin; Khweek, Arwa Abu; Hamilton, Kaitlin; Badr, Asmaa; Vaidya, Anup; Daily, Kylene; Gosu, Hawin; Anne, Midhun N. K.; Eltobgy, Mostafa; Dakhlallah, Duaa; Argwal, Sudha; Estfanous, Shady; Zhang, Xiaoli; Partida-Sánchez, Santiago; Gavrilin, Mikhail A.; Amer, Amal O.

doi:10.3389/fimmu.2019.02519

Cited by 52 publications

(55 citation statements)

References 90 publications

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“…Knockdown of caspase‐5 reduces IL‐1α release and cytokines associated with SASP such as IL‐6, MCP1, and IL‐8, suggesting that caspase‐5 is required for IL‐1α release during senescence in vitro. We also showed that IL‐6, KC, and TNF‐α are drastically reduced in the absence of caspase‐11 33 . Additionally, caspase‐11 −/− mice showed reduction in the level of IL‐1α and KC in response to MRSA infection 60 .…”

Section: Il‐1α Is a Direct Substrate Of Mouse Caspase‐11 And Human Camentioning

confidence: 53%

“…Recent study showed that at sublytic levels of inflammasome activation, and in the absence of pyroptotic cell death, gasdermin D pores mediate the release of IL‐1β or IL‐18 and other cytosolic proteins 84 . Notably, we have shown that the release of IL‐1β from macrophages in response to MSU was not accompanied by cell death 33 . Our findings are corroborated by recent reports describing how gasdermin forms pores within the intact plasma membrane, allowing the release of IL‐1β independently of cell death 85,86 .…”

Section: Non‐apoptotic Functions Of Caspase‐11 and Gasdermin Dmentioning

confidence: 62%

“…HMGB1 utilizes a variety of receptors to promote its signaling events, and LPS is sensed by TLR4, which uses both adapters to signal 35,36 . We have shown that caspase‐11 expression was not significantly hampered in the WT or the single knockout macrophages during stimulation with either HMGB1 or LPS, except when both MYD88 and TRIF were absent, indicating that either adapter was able to countervail for the deficient one in order to induce caspase‐11 33 . Certain diseases have been classified as an IL‐1β‐mediated condition such as gout since neutralizing antibodies to IL‐1β or the caspase‐1 inhibitor z‐YVAD significantly reduce inflammation and the production of other cytokines within the joints 37‐39 .…”

Section: Stimuli That Induce Caspase‐11 Expression and Activationmentioning

confidence: 89%

“…Recently, we have demonstrated that expression of caspase‐11 is induced by IL‐1β and IL‐1α via the IL‐1R/MYD88 33 . Indeed, single myd88 −/− , trif −/− , and myd88/ trif −/− , macrophages, 34 showed reduced caspase‐11 expression in response to IL‐1α and IL‐1β, or in combination, respectively 33 . Additionally, we have revealed that induction of caspase‐11 by LPS and HMGB1 is independent of IL‐1R.…”

Section: Stimuli That Induce Caspase‐11 Expression and Activationmentioning

confidence: 99%

“…Induction of caspase‐11 expression by released IL‐1β and IL‐1α could prime immune cells for inflammasome activation by subsequent insults including monosodium urate (MSU). Thus, preventing the expression of caspase‐11 in gout‐prone individuals may prevent the instigation of tissue damage 33 . Additionally, we have shown that house dust mites (HDM) induce caspase‐11 expression in bone marrow‐derived macrophages and in C57BL/6 mice (Abu Khweek et al under review).…”

Section: Stimuli That Induce Caspase‐11 Expression and Activationmentioning

confidence: 99%

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Pyroptotic and non‐pyroptotic effector functions of caspase‐11

Khweek

Amer

2020

Immunological Reviews

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Innate immune cells, epithelial cells, and many other cell types are capable of detecting infection or tissue injury, thus mounting regulated immune response. Inflammasomes are highly sophisticated and effective orchestrators of innate immunity. These oligomerized multiprotein complexes are at the center of various innate immune pathways, including modulation of the cytoskeleton, production and maturation of cytokines, and control of bacterial growth and cell death. Inflammasome assembly often results in caspase‐1 activation, which is an inflammatory caspase that is involved in pyroptotic cell death and release of inflammatory cytokines in response to pathogen patterns and endogenous danger stimuli. However, the nature of stimuli and inflammasome components are diverse. Caspase‐1 activation mediated release of mature IL‐1β and IL‐18 in response to canonical stimuli initiated by NOD‐like receptor (NLR), and apoptosis‐associated speck‐like protein containing a caspase recruitment domain (ASC). On the other hand, caspase‐11 delineates a non‐canonical inflammasome that promotes pyroptotic cell death and non‐pyroptotic functions in response to non‐canonical stimuli. Caspase‐11 in mice and its homologues in humans (caspase‐4/5) belong to caspase‐1 family of cysteine proteases, and play a role in inflammation. Knockout mice provided new genetic tools to study inflammatory caspases and revealed the role of caspase‐11 in mediating septic shock in response to lethal doses of lipopolysaccharide (LPS). Recognition of LPS mediates caspase‐11 activation, which promotes a myriad of downstream effects that include pyroptotic and non‐pyroptotic effector functions. Therefore, the physiological functions of caspase‐11 are much broader than its previously established roles in apoptosis and cytokine maturation. Inflammation induced by exogenous or endogenous agents can be detrimental and, if excessive, can result in organ and tissue damage. Consequently, the existence of sophisticated mechanisms that tightly regulate the specificity and sensitivity of inflammasome pathways provides a fine‐tuning balance between adequate immune response and minimal tissue damage. In this review, we summarize effector functions of caspase‐11.

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Section: Il‐1α Is a Direct Substrate Of Mouse Caspase‐11 And Human Camentioning

confidence: 53%

Section: Non‐apoptotic Functions Of Caspase‐11 and Gasdermin Dmentioning

confidence: 62%

Section: Stimuli That Induce Caspase‐11 Expression and Activationmentioning

confidence: 89%

Section: Stimuli That Induce Caspase‐11 Expression and Activationmentioning

confidence: 99%

Section: Stimuli That Induce Caspase‐11 Expression and Activationmentioning

confidence: 99%

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Pyroptotic and non‐pyroptotic effector functions of caspase‐11

Khweek

Amer

2020

Immunological Reviews

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Dying to Defend: Neutrophil Death Pathways and their Implications in Immunity

Tu,

Ren,

Jiang

et al. 2023

Advanced Science

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Neutrophils, accounting for ≈70% of human peripheral leukocytes, are key cells countering bacterial and fungal infections. Neutrophil homeostasis involves a balance between cell maturation, migration, aging, and eventual death. Neutrophils undergo different death pathways depending on their interactions with microbes and external environmental cues. Neutrophil death has significant physiological implications and leads to distinct immunological outcomes. This review discusses the multifarious neutrophil death pathways, including apoptosis, NETosis, pyroptosis, necroptosis, and ferroptosis, and outlines their effects on immune responses and disease progression. Understanding the multifaceted aspects of neutrophil death, the intersections among signaling pathways and ramifications of immunity will help facilitate the development of novel therapeutic methods.

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Inflammasome: structure, biological functions, and therapeutic targets

Dai,

Zhou,

Shi

2023

MedComm

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Inflammasomes are a group of protein complex located in cytoplasm and assemble in response to a wide variety of pathogen‐associated molecule patterns, damage‐associated molecule patterns, and cellular stress. Generally, the activation of inflammasomes will lead to maturation of proinflammatory cytokines and pyroptotic cell death, both associated with inflammatory cascade amplification. A sensor protein, an adaptor, and a procaspase protein interact through their functional domains and compose one subunit of inflammasome complex. Under physiological conditions, inflammasome functions against pathogen infection and endogenous dangers including mtROS, mtDNA, and so on, while dysregulation of its activation can lead to unwanted results. In recent years, advances have been made to clarify the mechanisms of inflammasome activation, the structural details of them and their functions (negative/positive) in multiple disease models in both animal models and human. The wide range of the stimuli makes the function of inflammasome diverse and complex. Here, we review the structure, biological functions, and therapeutic targets of inflammasomes, while highlight NLRP3, NLRC4, and AIM2 inflammasomes, which are the most well studied. In conclusion, this review focuses on the activation process, biological functions, and structure of the most well‐studied inflammasomes, summarizing and predicting approaches for disease treatment and prevention with inflammasome as a target. We aim to provide fresh insight into new solutions to the challenges in this field.

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Caspase-11 Mediates Neutrophil Chemotaxis and Extracellular Trap Formation During Acute Gouty Arthritis Through Alteration of Cofilin Phosphorylation

Cited by 52 publications

References 90 publications

Pyroptotic and non‐pyroptotic effector functions of caspase‐11

Pyroptotic and non‐pyroptotic effector functions of caspase‐11

Dying to Defend: Neutrophil Death Pathways and their Implications in Immunity

Inflammasome: structure, biological functions, and therapeutic targets

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