Fra1 Controls Rheumatoid Factor Autoantibody Production by Bone Marrow Plasma Cells and the Development of Autoimmune Bone Loss

Grötsch, Bettina; Lux, Anja; Rombouts, Yoann; Hoffmann, Anna-Carin; Andreev, Darja; Nimmerjahn, Falk; Xiang, Wei; Scherer, Hans Ulrich; Schett, Georg; Bözec, Aline

doi:10.1002/jbmr.3705

Cited by 10 publications

(8 citation statements)

References 46 publications

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“…However, subsequent studies have pointed out that Fra-1 can inhibit the production and development of plasma cells by regulating the direct combination with the Prdm1/Bimp1(PR/SET Domain 1/B lymphocyte induced maturation protein 1) promoter ( 142 ). In addition, the activation of B cells by TD antigen can reduce the expression of Fra-1, which can control the production of IgG-RF and inhibit the activation of osteoclasts driven by immune complexes ( 143 ). Therefore Fra-1 may be used as a regulator to block the negative effects of autoimmunity by inhibiting the formation of immune complexes.…”

Section: Fra-1-mediated Immune Regulationmentioning

confidence: 99%

“…Different from the absence of other AP-1 members, c-Fos deficient mice have more severe arthritis ( 177 ). Overexpression of Fra-1 in CD4 + T cells can bind to JunB as a downstream target of Stat3 to induce Th17 cell differentiation and promote autoimmune arthritis ( 143 ). Inhibition of AP-1 activity can prevent acute graft-versus-host disease (aGVHD) by altering the differentiation of CD4 + T cells, such as reduced Th17/Th1 population and increased Treg population ( 163 ).…”

Section: Immune-related Diseasesmentioning

confidence: 99%

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The Fra-1: Novel role in regulating extensive immune cell states and affecting inflammatory diseases

Zhou

Chen

et al. 2022

Front. Immunol.

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Fra-1(Fos-related antigen1), a member of transcription factor activator protein (AP-1), plays an important role in cell proliferation, apoptosis, differentiation, inflammation, oncogenesis and tumor metastasis. Accumulating evidence suggest that the malignancy and invasive ability of tumors can be significantly changed by directly targeting Fra-1. Besides, the effects of Fra-1 are gradually revealed in immune and inflammatory settings, such as arthritis, pneumonia, psoriasis and cardiovascular disease. These regulatory mechanisms that orchestrate immune and non-immune cells underlie Fra-1 as a potential therapeutic target for a variety of human diseases. In this review, we focus on the current knowledge of Fra-1 in immune system, highlighting its unique importance in regulating tissue homeostasis. In addition, we also discuss the possible critical intervention strategy in diseases, which also outline future research and development avenues.

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Section: Fra-1-mediated Immune Regulationmentioning

confidence: 99%

Section: Immune-related Diseasesmentioning

confidence: 99%

The Fra-1: Novel role in regulating extensive immune cell states and affecting inflammatory diseases

Zhou

Chen

et al. 2022

Front. Immunol.

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“…Importantly, osteoclasts express several Fcγ receptors and IgG containing ICs can activate osteoclasts and increase bone loss independently of the antigen specificity. [31][32][33] The osteoclast activating effect of IgGs appears to be dependent on the Fc glycosylation status, IgG isotype and the different distribution of Fcγ receptors in physiological compared with inflammatory conditions. 34 If the ACPA containing ICs exert similar Fc-dependent effects, it still remains to be demonstrated.…”

Section: Pathogenic Effects Of Acpas Macrophage Activationmentioning

confidence: 99%

Current view on the pathogenic role of anti-citrullinated protein antibodies in rheumatoid arthritis

2021

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Epidemiological findings suggest a potential role for anti-citrullinated protein antibodies (ACPAs) in rheumatoid arthritis (RA) pathogenesis. ACPA-positive RA is associated with unique genetical and environmental risk factors, in contrast to seronegative RA. ACPA-positive healthy individuals are at risk of developing RA and can develop joint pain and bone loss already before disease onset. ACPA injection triggered bone loss and pain-like behaviour in mice and, in the presence of additional arthritis inducers, exacerbated joint inflammation. In cell culture experiments, ACPAs could bind to and modulate a variety of cellular targets, such as macrophages, osteoclasts, synovial fibroblasts, neutrophil granulocytes, mast cells, dendritic cells and platelets, further underlying a potential role for these autoantibodies in triggering pathogenic pathways and providing clues for their mechanisms of action. Patient-derived ACPA clones have been characterised by unique cellular effects and multiple ways to act on the target cells. ACPAs might directly induce stimulatory signals by ligating key citrullinated cell surface molecules or, alternatively, act as immune complexes on Fc receptors and potentially other molecules that recognise carbohydrate moieties. On the contrary to experimentally manufactured ACPA clones, patient-derived ACPAs are highly promiscuous and cross-reactive, suggesting a simultaneous binding to a range of functionally relevant and irrelevant targets. Moreover, several ACPA clones recognise carbamylated or acetylated targets as well. These features complicate the identification and description of ACPA-induced pathogenic mechanisms. In the current review, we summarise recent data on the functional properties of patient-derived ACPAs and present mechanistic models on how these antibodies might contribute to RA pathogenesis.

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“…Most effects of antibodies on osteoclasts seem to be mediated by binding of complexed IgG (e. g. immune complexes) to low affinity FcγRs. Mice with increased autoantibody formation caused by the loss of B cell checkpoints display systemic osteoporosis due to osteoclast activation by immune complexes [11,12]. Stimulation of osteoclasts with serum from these mice resulted in increased osteoclast formation and resorption activity.…”

Section: Fc-mediated Effects Of Antibodies On Osteoclastsmentioning

confidence: 99%

Effects of Autoantibodies on Osteoclasts

Sokolova

Steffen

2021

Osteologie

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The balance between bone forming osteoblasts and bone resorbing osteoclasts can be disturbed in autoimmune diseases resulting in local and systemic bone loss. It was long time believed that autoantibodies only indirectly contribute to bone loss by fueling the overall inflammation. However, in the last decade, more and more evidence emerged that autoantibodies and immune complexes directly activate osteoclasts and pre-osteoclasts by binding to Fcγ receptors (FcγRs) on the (pre)-osteoclast cell surface. This pro-osteoclastogenic effect seems to be dependent on the absence of sialic acid in the IgG Fc glycan, which is a typical feature of many autoantibodies. Clinical studies revealed the importance of autoantibody-mediated bone loss mainly in rheumatoid arthritis, but also in other diseases, such as celiac disease. In summary, the gained knowledge about autoantibody-mediated bone loss helps to better understand bone pathologies of autoimmune diseases. However, studies are still relatively limited and more research is needed to fully understand the impact of autoantibodies on bone and to develop future therapeutic strategies.

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Fra1 Controls Rheumatoid Factor Autoantibody Production by Bone Marrow Plasma Cells and the Development of Autoimmune Bone Loss

Cited by 10 publications

References 46 publications

The Fra-1: Novel role in regulating extensive immune cell states and affecting inflammatory diseases

The Fra-1: Novel role in regulating extensive immune cell states and affecting inflammatory diseases

Current view on the pathogenic role of anti-citrullinated protein antibodies in rheumatoid arthritis

Effects of Autoantibodies on Osteoclasts

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