Your search keyword '"Jennifer Müller"' showing total 3 results

1. Siglec-G Deficiency Leads to Autoimmunity in Aging C57BL/6 Mice

Author

Benjamin Lunz, Falk Nimmerjahn, Inessa Schwab, Andreas Acs, Jennifer Müller, Lars Nitschke, and Christoph Daniel

Subjects

CD4-Positive T-Lymphocytes, Male, Aging, Mice, Inbred MRL lpr, Immunology, Gene Expression, Receptors, Antigen, B-Cell, Autoimmunity, Biology, Immune tolerance, Mice, Glomerulonephritis, Lectins, Immune Tolerance, medicine, Animals, Immunology and Allergy, Crosses, Genetic, B cell, Autoantibodies, Mice, Knockout, Sialic Acid Binding Immunoglobulin-like Lectins, Autoimmune disease, B-Lymphocytes, Receptors, IgG, CD22, Autoantibody, Germinal center, Dendritic cell, respiratory system, Germinal Center, medicine.disease, Mice, Inbred C57BL, B-1 cell, medicine.anatomical_structure, Female

Abstract

Siglec-G, a member of the sialic acid–binding Ig-like lectin (Siglec) family, is expressed on B cell and dendritic cell surfaces. It acts as an inhibitory coreceptor and modulates B cell activation, especially on B1 cells, as Siglec-G–deficient mice show mainly a B1 cell–restricted phenotype resulting in increased B1 cell numbers. Although higher B1 cell numbers are discussed to be associated with autoimmunity, loss of Siglec-G does not result in autoimmune disease in BALB/c mice. However, there is evidence from Siglec-G × CD22 double-deficient mice and Siglec-G−/− mice on an autoimmune-prone MRL/lpr background that Siglec-G is important to maintain tolerance in B cells. In this study, we analyzed the role of Siglec-G in induction and maintenance of B cell tolerance on C57BL/6 background and in the FcγRIIb-deficient background. We find that aging Siglec-G–deficient and Siglec-G × FcγRIIb double-deficient mice develop an autoimmune phenotype with elevated autoantibody levels and mild glomerulonephritis. Aging Siglec-G–deficient mice have elevated numbers of plasma cells and germinal center B cells, as well as a higher number of activated CD4 T cells, which likely all contribute to autoantibody production. Additional loss of the inhibitory receptor FcγRIIb in Siglec-G−/− mice does not result in exacerbation of disease. These results indicate that Siglec-G is important to maintain tolerance in B cells and prevent autoimmunity.

Published

2015

2. A Balance between B Cell Receptor and Inhibitory Receptor Signaling Controls Plasma Cell Differentiation by Maintaining Optimal Ets1 Levels

Author

Jane Parnes, Thomas F. Tedder, Jennifer Müller, Jessica M. Mayeux, Lisa Russell, Wei Luo, Robert C. Rickert, Andrew Getahun, John C. Cambier, Lars Nitschke, Anne B. Satterthwaite, Toni Gutierrez, and Lee Ann Garrett-Sinha

Subjects

Cellular differentiation, Immunology, CD22, B-cell receptor, Biology, medicine.anatomical_structure, Cell surface receptor, LYN, hemic and lymphatic diseases, Plasma cell differentiation, medicine, Cancer research, Immunology and Allergy, Signal transduction, B cell

Abstract

Signaling through the BCR can drive B cell activation and contribute to B cell differentiation into Ab-secreting plasma cells. The positive BCR signal is counterbalanced by a number of membrane-localized inhibitory receptors that limit B cell activation and plasma cell differentiation. Deficiencies in these negative signaling pathways may cause autoantibody generation and autoimmune disease in both animal models and human patients. We have previously shown that the transcription factor Ets1 can restrain B cell differentiation into plasma cells. In this study, we tested the roles of the BCR and inhibitory receptors in controlling the expression of Ets1 in mouse B cells. We found that Ets1 is downregulated in B cells by BCR or TLR signaling through a pathway dependent on PI3K, Btk, IKK2, and JNK. Deficiencies in inhibitory pathways, such as a loss of the tyrosine kinase Lyn, the phosphatase Src homology region 2 domain–containing phosphatase 1 (SHP1) or membrane receptors CD22 and/or Siglec-G, result in enhanced BCR signaling and decreased Ets1 expression. Restoring Ets1 expression in Lyn- or SHP1-deficient B cells inhibits their enhanced plasma cell differentiation. Our findings indicate that downregulation of Ets1 occurs in response to B cell activation via either BCR or TLR signaling, thereby allowing B cell differentiation and that the maintenance of Ets1 expression is an important function of the inhibitory Lyn → CD22/SiglecG → SHP1 pathway in B cells.

Published

2014

3. A balance between BCR and inhibitory receptor signaling controls plasma cell differentiation by maintaining optimal Ets1 levels (BA2P.120)

Author

Wei Luo, Jessica Mayeux, Toni Gutierrez, Andy Getahun, Jennifer Müller, Thomas Tedder, Shu-Hsia Chen, Robert Rickert, Lars Nitschke, John Cambier, Anne Satterthwaite, and Lee Ann Garrett-Sinha

Subjects

Immunology, Immunology and Allergy

Abstract

Signaling through the B cell receptor (BCR) can drive B cell activation and contribute to B cell differentiation into antibody-secreting plasma cells. The positive BCR activation signal is counterbalanced by a number of membrane-localized inhibitory receptors that limit B cell activation and plasma cell differentiation. Deficiencies in these negative signaling pathways may cause autoantibody generation and autoimmune disease in both animal models and human patients. We have previously shown that the transcription factor Ets1 can restrain B cell differentiation into plasma cells. Here, we tested the roles of the BCR and inhibitory receptors in controlling the expression of Ets1 in B cells. We found that Ets1 is down regulated in B cells by BCR or TLR signaling through a pathway dependent on PI3 kinase, Btk, IKK2 and JNK. Deficiencies in inhibitory pathways, such as a loss of the tyrosine kinase Lyn, the phosphatase SHP1 or membrane receptors CD22 or Siglec-G, result in enhanced BCR signaling and decreased Ets1 expression. Restoring Ets1 expression in Lyn- or SHP1-deficient B cells inhibits their enhanced plasma cell differentiation. Our findings suggest that the maintenance of Ets1 expression is an important function of the inhibitory Lyn -- CD22/SiglecG -- SHP1 pathway in B cells.

Published

2014