Increased IgG on cell‐derived plasma microparticles in systemic lupus erythematosus is associated with autoantibodies and complement activation

Nielsen, Christoffer Tandrup; Østergaard, Ole; Stener, Line; Iversen, Line V.; Truedsson, Lennart; Gullstrand, Birgitta; Jacobsen, Søren; Heegaard, Niels H. H.

doi:10.1002/art.34381

Cited by 147 publications

(156 citation statements)

References 51 publications

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“…Although immunoglobulin and complement proteins have been detected on the surface of microparticles from apoptotic cells 14 and microparticles isolated from patients with inflammatory diseases, [15][16][17] these previous studies did not Microparticles from the supernatant of unmanipulated or CsA-treated cells were exposed to serum, and C3 deposition on the microparticles was assessed by Western blot analysis using a polyclonal antibody to C3 and a monoclonal antibody to C3d. The a92 band of C3 (representing the iC3b form) and C3d were readily detected on microparticles from CsA-treated cells that were exposed to serum (MP, microparticle; NMS, normal mouse serum; S, serum).…”

Section: Discussionmentioning

confidence: 91%

Cyclosporine Induces Endothelial Cell Release of Complement-Activating Microparticles

Renner¹,

Klawitter²,

Goldberg³

et al. 2013

Journal of the American Society of Nephrology

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Defective control of the alternative pathway of complement is an important risk factor for several renal diseases, including atypical hemolytic uremic syndrome. Infections, drugs, pregnancy, and hemodynamic insults can trigger episodes of atypical hemolytic uremic syndrome in susceptible patients. Although the mechanisms linking these clinical events with disease flares are unknown, recent work has revealed that each of these clinical conditions causes cells to release microparticles. We hypothesized that microparticles released from injured endothelial cells promote intrarenal complement activation. Calcineurin inhibitors cause vascular and renal injury and can trigger hemolytic uremic syndrome. Here, we show that endothelial cells exposed to cyclosporine in vitro and in vivo release microparticles that activate the alternative pathway of complement. Cyclosporine-induced microparticles caused injury to bystander endothelial cells and are associated with complement-mediated injury of the kidneys and vasculature in cyclosporine-treated mice. Cyclosporine-induced microparticles did not bind factor H, an alternative pathway regulatory protein present in plasma, explaining their complement-activating phenotype. Finally, we found that in renal transplant patients, the number of endothelial microparticles in plasma increases 2 weeks after starting tacrolimus, and treatment with tacrolimus associated with increased C3 deposition on endothelial microparticles in the plasma of some patients. These results suggest that injury-associated release of endothelial microparticles is an important mechanism by which systemic insults trigger intravascular complement activation and complement-dependent renal diseases.

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Section: Discussionmentioning

confidence: 91%

Cyclosporine Induces Endothelial Cell Release of Complement-Activating Microparticles

Renner¹,

Klawitter²,

Goldberg³

et al. 2013

Journal of the American Society of Nephrology

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“…This is not the first time an autoantigen has been identified on MVs. Studies examining other autoimmune diseases including rheumatoid arthritis and systemic lupus erythematosus have found that autoantigens are expressed on MVs and that these MVs can form potent inflammatory complexes containing autoantibodies (55,56). This phenomenon may also contribute to inflammation in GPA, although more research is required to determine whether these complexes form when MVs are produced from a PR3-expressing cell.…”

Section: Discussionmentioning

confidence: 99%

Proteinase 3 Is a Phosphatidylserine-binding Protein That Affects the Production and Function of Microvesicles

Martin¹,

Kantari‐Mimoun²,

Yin³

et al. 2016

Journal of Biological Chemistry

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Proteinase 3 (PR3), the autoantigen in granulomatosis with polyangiitis, is expressed at the plasma membrane of resting neutrophils, and this membrane expression increases during both activation and apoptosis. Using surface plasmon resonance and protein-lipid overlay assays, this study demonstrates that PR3 is a phosphatidylserine-binding protein and this interaction is dependent on the hydrophobic patch responsible for membrane anchorage. Molecular simulations suggest that PR3 interacts with phosphatidylserine via a small number of amino acids, which engage in long lasting interactions with the lipid heads. As phosphatidylserine is a major component of microvesicles (MVs), this study also examined the consequences of this interaction on MV production and function. PR3-expressing cells produced significantly fewer MVs during both activation and apoptosis, and this reduction was dependent on the ability of PR3 to associate with the membrane as mutating the hydrophobic patch restored MV production. Functionally, activation-evoked MVs from PR3-expressing cells induced a significantly larger respiratory burst in human neutrophils compared with control MVs. Conversely, MVs generated during apoptosis inhibited the basal respiratory burst in human neutrophils, and those generated from PR3-expressing cells hampered this inhibition. Given that membrane expression of PR3 is increased in patients with granulomatosis with polyangiitis, MVs generated from neutrophils expressing membrane PR3

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“…Similarly, plasma EVs from systemic lupus erythematous (SLE) were shown to not only contain self antigens (69,70), but also to interact with IgG, IgM, and complement proteins. However, it was not clear whether these interactions represent true immune complexes (71)(72)(73). Additionally, EVs enhance autoimmune phenotypes through secretion or surface expression of proinflammatory cytokines that promote an inflammatory environment and autoreactive T cell survival (74,75).…”

Section: The Role Of Evs In Autoimmunitymentioning

confidence: 99%

Regulation of chronic inflammatory and immune processes by extracellular vesicles

Robbins

Dorronsoro

Booker

2016

Journal of Clinical Investigation

224

195

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Increased IgG on cell‐derived plasma microparticles in systemic lupus erythematosus is associated with autoantibodies and complement activation

Cited by 147 publications

References 51 publications

Cyclosporine Induces Endothelial Cell Release of Complement-Activating Microparticles

Cyclosporine Induces Endothelial Cell Release of Complement-Activating Microparticles

Proteinase 3 Is a Phosphatidylserine-binding Protein That Affects the Production and Function of Microvesicles

Regulation of chronic inflammatory and immune processes by extracellular vesicles

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