Neutrophils Slow Disease Progression in Murine Lupus via Modulation of Autoreactive Germinal Centers

Bird, Anna; Chang, Martin; Barnard, Jennifer; Goldman, Bruce; Meednu, Nida; Rangel-Moreno, Javier; Anolik, Jennifer H.

doi:10.4049/jimmunol.1700354

Cited by 26 publications

(34 citation statements)

References 54 publications

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“…Cxcr2 nor Cxcr4-factors mediating neutrophil migration to sites of infection and clearance (respectively)-were differentially expressed (d.n.s) 206 . These chemokine receptor changes are consistent with the changing frequency of neutrophils in the spleen observed in our previously published work 201 . 215 .…”

Section: Neutrophil Transcription Of Immunologic Mediators Changes Sisupporting

confidence: 92%

The role of neutrophils in the pathogenesis of systemic lupus erythematosus

Smith

Kaplan²

2015

Current Opinion in Rheumatology

125

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Section: Neutrophil Transcription Of Immunologic Mediators Changes Sisupporting

confidence: 92%

The role of neutrophils in the pathogenesis of systemic lupus erythematosus

Smith

Kaplan²

2015

Current Opinion in Rheumatology

125

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“…Despite the extensive literature supporting a role of neutrophils in driving exaggerated B‐cell responses that can lead to autoimmune and neoplastic disease development, it is important to highlight that evidence that neutrophils may inhibit B‐cell responses is also emerging. For example, neutrophils have been proposed to inhibit IgA production by B cells in a mouse model of sublingual immunization, or to inhibit germinal centre B‐cell formation during the early stages of murine lupus development . Similarly, during the early phases of the humoral response after local Staphylococcus aureus immunization and infection, murine neutrophils have been shown to establish F‐actin‐mediated intercellular contacts with B cells within the lymph nodes, and in turn suppress antibody production via transforming growth factor ‐ β 1 production .…”

Section: Neutrophils and B Cellsmentioning

confidence: 99%

Recent advances on the crosstalk between neutrophils and B or T lymphocytes

et al. 2018

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An increasing body of literature supports a role for neutrophils as players in the orchestration of adaptive immunity. During acute and chronic inflammatory conditions, neutrophils rapidly migrate not only to sites of inflammation, but also to draining lymph nodes and spleen, where they engage bidirectional interactions with B-and T-lymphocyte subsets. Accordingly, a relevant role of neutrophils in modulating B-cell responses under homeostatic conditions has recently emerged. Moreover, specialized immunoregulatory properties towards B or T cells acquired by distinct neutrophil populations, originating under pathological conditions, have been consistently described. In this article, we summarize the most recent data from human studies and murine models on the ability of neutrophils to modulate adaptive immune responses under physiological and pathological conditions and the mechanisms behind these processes.

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“…Animal models of lupus have not supported a pathogenic role for neutrophils in SLE pathogenesis; rather, data has supported a regulatory or neutral role for neutrophils. Antibody mediated depletion of neutrophils early in disease increased autoantibody titers and glomerulonephritis in the NZB/W model [57, 58]. However, neutrophil depletion did not alter autoantibody responses nor renal pathology in established disease [57].…”

Section: Discussionmentioning

confidence: 99%

“…Antibody mediated depletion of neutrophils early in disease increased autoantibody titers and glomerulonephritis in the NZB/W model [57, 58]. However, neutrophil depletion did not alter autoantibody responses nor renal pathology in established disease [57]. Conditional deletion of neutrophils in mice subjected to the PIL model resulted in increased antinuclear antibody responses [23].…”

Section: Discussionmentioning

confidence: 99%

Murine lupus is Neutrophil Elastase-independent in the MRL.Fas^lpr model

Gordon

Tilstra

Marinov

et al. 2019

Preprint

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AbstractLoss of tolerance to nuclear antigens and multisystem tissue destruction is a hallmark of systemic lupus erythematosus (SLE). Although the source of autoantigen in lupus remains elusive, a compelling hypothetical source is dead cell debris that drives autoimmune activation. Prior reports suggest that neutrophil extracellular traps (NETs) and their associated death pathway, NETosis, are sources of autoantigen in SLE. However, others and we have shown that inhibition of NETs by targeting the NADPH oxidase complex and peptidylarginine deiminase 4 (PADI4) did not ameliorate disease in spontaneous murine models of SLE. Furthermore, myeloperoxidase and PADI4 deletion did not inhibit induced lupus. Since NET formation may occur independently of any one mediator, to address this controversy, we genetically deleted an additional important mediator of NETs and neutrophil effector function, neutrophil elastase (ELANE), in the MRL.Faslpr model of SLE. ELANE deficiency, and by extension ELANE-dependent NETs, had no effect on SLE nephritis, dermatitis, anti-self response, or immune composition in MRL.Faslpr mice. Taken together with prior data from our group and others, these data further challenge the paradigm that NETs and neutrophils are pathogenic in SLE.

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Neutrophils Slow Disease Progression in Murine Lupus via Modulation of Autoreactive Germinal Centers

Cited by 26 publications

References 54 publications

The role of neutrophils in the pathogenesis of systemic lupus erythematosus

The role of neutrophils in the pathogenesis of systemic lupus erythematosus

Recent advances on the crosstalk between neutrophils and B or T lymphocytes

Murine lupus is Neutrophil Elastase-independent in the MRL.Fas^lpr model

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Neutrophils Slow Disease Progression in Murine Lupus via Modulation of Autoreactive Germinal Centers

Cited by 26 publications

References 54 publications

The role of neutrophils in the pathogenesis of systemic lupus erythematosus

The role of neutrophils in the pathogenesis of systemic lupus erythematosus

Recent advances on the crosstalk between neutrophils and B or T lymphocytes

Murine lupus is Neutrophil Elastase-independent in the MRL.Faslpr model

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Murine lupus is Neutrophil Elastase-independent in the MRL.Fas^lpr model