Interaction of kindlin-3 and β2-integrins differentially regulates neutrophil recruitment and NET release in mice

Xu, Zhen; Gao, Juan; White, Gilbert; Chen, Fangyuan; Ma, Yanqing

doi:10.1182/blood-2015-03-636720

Cited by 34 publications

(41 citation statements)

References 25 publications

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“…These pathways include activation by integrins (complement receptor) and Toll-like receptors (14)(15)(16). Chemokine receptors are necessary for integrin activation and signaling (10,17). Integrins generate signals that elicit NETosis in response to bacteria, and NETs are not produced when integrins are deficient, such as in leukocyte adhesion deficiency (18).…”

Section: Inducers Of Net Formationmentioning

confidence: 99%

Neutrophil extracellular traps — the dark side of neutrophils

Sørensen¹,

Borregaard

2016

Journal of Clinical Investigation

382

318

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Section: Inducers Of Net Formationmentioning

confidence: 99%

Neutrophil extracellular traps — the dark side of neutrophils

Sørensen¹,

Borregaard

2016

Journal of Clinical Investigation

382

318

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“…Inhibition of neutrophil recruitment and NET release by disrupting the cross-talk between kindlin-3 and β2-integrin, is also an interesting therapeutic avenue 159 . CXCL5 could also be targeted to restrict pathogenic neutrophil infiltration in T H 17-mediated autoimmune diseases, especially crescentic glomerulonephritis, while retaining the protective function of neutrophils against invading pathogens 132 .…”

Section: Potential Therapeutic Modulation Of Netosismentioning

confidence: 99%

The role of neutrophils and NETosis in autoimmune and renal diseases

2016

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Systemic autoimmune diseases are a group of disorders characterized by a failure in self-tolerance to a wide variety of autoantigens. In genetically predisposed individuals, these diseases occur as a multistep process in which environmental factors have key roles in the development of abnormal innate and adaptive immune responses. Experimental evidence collected in the past decade suggests that neutrophils — the most abundant type of white blood cell — might have an important role in the pathogenesis of these diseases by contributing to the initiation and perpetuation of immune dysregulation through the formation of neutrophil extracellular traps (NETs), synthesis of proinflammatory cytokines and direct tissue damage. Many of the molecules externalized through NET formation are considered to be key autoantigens and might be involved in the generation of autoimmune responses in predisposed individuals. In several systemic autoimmune diseases, the imbalance between NET formation and degradation might increase the half-life of these lattices, which could enhance the exposure of the immune system to modified autoantigens and increase the capacity for NET-induced organ damage. This Review details the role of neutrophils and NETs in the pathophysiology of systemic autoimmune diseases, including their effect on renal damage, and discusses neutrophil targets as potential novel therapies for these diseases.

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“…Neutrophil recruitment to necrotic tissues is mediated by high-mobility group box 1 (HMGB1) and its receptor, receptor for advanced glycation end products (RAGE) [31]; here, a potential link to integrin-dependent neutrophil recruitment may exist, as RAGE interacts with the β2-integrin Mac-1 [32, 33]. An important player in leukocyte integrin activation is kindlin-3, which interacts with the cytoplasmic tail of β2-integrins [34], and the absence of which causes leukocyte adhesion deficiency (LAD) Type III [35]. In genetically modified mice that express a mutant form of kindlin-3 that is incapable of interacting with integrins, neutrophil adhesion and recruitment in the course of systemic inflammation is decreased [34].…”

Section: Novel Regulatory Mechanisms Of Neutrophil Adhesionmentioning

confidence: 99%

Regulation of tissue infiltration by neutrophils

Subramanian

Mitroulis

Hajishengallis

et al. 2016

Current Opinion in Hematology

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Purpose of review Neutrophils have traditionally been viewed in the context of acute infection and inflammation forming the first line of defence against invading pathogens. Neutrophil trafficking to the site of inflammation requires adhesion and transmigration through blood vessels, which is orchestrated by adhesion molecules, such as β2- and β1-integrins, chemokines and cytokines. This review focuses on recent advances in understanding the regulators of neutrophil recruitment during inflammation in both acute and chronic settings. Recent findings Recent findings suggest that besides the established pathways of selectin or chemokine-mediated integrin activation, signaling by distinct TLRs (especially TLR2, TLR4 and TLR5) can activate integrin-dependent neutrophil adhesion. Moreover, the integrin α3β1 has been vitally implicated as a new player in neutrophil recruitment and TLR-mediated responses in septic inflammation. Furthermore, several endogenous inhibitory mechanisms of leukocyte recruitment have been identified, including the secreted molecules Del-1, PTX3, and GDF-15, which block distinct steps of the leukocyte adhesion cascade, as well as novel regulatory signaling pathways, involving the protein kinase AKT1 and IFN-λ2/IL-28A. Summary The leukocyte adhesion cascade is a tightly regulated process, subjected to both positive and negative regulators. Dysregulation of this process and hence neutrophil recruitment can lead to the development of inflammatory and autoimmune diseases.

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Interaction of kindlin-3 and β2-integrins differentially regulates neutrophil recruitment and NET release in mice

Cited by 34 publications

References 25 publications

Neutrophil extracellular traps — the dark side of neutrophils

Neutrophil extracellular traps — the dark side of neutrophils

The role of neutrophils and NETosis in autoimmune and renal diseases

Regulation of tissue infiltration by neutrophils

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