Abstract

B cells are involved in many autoimmune diseases. CD19 regulates B cell functions in vivo that are important in autoimmunity. Extensive studies in vitro have identified multiple signaling pathways, linked to specific CD19 cytoplasmic tyrosines, that may mediate CD19 function but their relative importance in vivo is unknown. We have developed a system for studying CD19 tyrosine-based signaling in vivo. Mice that are deficient in CD19 lack peritoneal B 1 and marginal zone B cells and respond poorly to T-independent antigens. We reconstituted these functions with an unmutated CD19 transgene, but a construct with mutation of all cytoplasmic tyrosines completely failed to do so, demonstrating the dependence of these B cell functions on CD19 tyrosine signaling. To determine the relevance in vivo of the multiple pathways that have been linked to particular tyrosines and the molecules that bind them in vitro, we produced four transgenes each containing mutations of distinct pairs of homologous CD19 tyrosines. Founder lines for each have been crossed onto the CD19-/- background. We initially studied the role of Y482 and Y513, which bind Lyn and phosphatidylinositol 3-kinase (PI3K), and found an absolute requirement for these in all in vivo CD19 functions tested. The likely mechanism is the abrogation of phosphorylation of all CD19 tyrosines by these mutations. This finding establishes that targeting particular CD19 tyrosines can modulate B cell responses in vivo. We propose to: 1) Identify the CD19 structures that control phosphorylation of the molecule, as these would be targets for global control of CD19 function, 2) Determine the role of binding of cytoplasmic molecules to particular CD19 tyrosines, as these mediate CD19 function, 3) Determine which downstream pathways are controlled by particular CD19 tyrosines in vivo, as these would be identified as regulating important B cell functions, and 4) Determine the role of CD19 tyrosine-based signaling in a mouse model of lupus, to test the hypothesis that targeting specific CD19 tyrosines could be used for therapeutic manipulation of B cells in autoimmune disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI042265-06
Application #
6622034
Study Section
Experimental Immunology Study Section (EI)
Program Officer
Mallia, Conrad M
Project Start
1998-01-01
Project End
2007-01-31
Budget Start
2003-02-01
Budget End
2004-01-31
Support Year
6
Fiscal Year
2003
Total Cost
$287,000
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
063690705
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Myers, Riley C; King, R Glenn; Carter, Robert H et al. (2013) Lymphotoxin ?1?2 expression on B cells is required for follicular dendritic cell activation during the germinal center response. Eur J Immunol 43:348-59
You, Yuying; Myers, Riley C; Freeberg, Larry et al. (2011) Marginal zone B cells regulate antigen capture by marginal zone macrophages. J Immunol 186:2172-81
You, Yuying; Zhao, Hong; Wang, Yue et al. (2009) Cutting edge: Primary and secondary effects of CD19 deficiency on cells of the marginal zone. J Immunol 182:7343-7
Carter, Robert H; Myers, Riley (2008) Germinal center structure and function: lessons from CD19. Semin Immunol 20:43-8
Wang, Yue; Carter, Robert H (2005) CD19 regulates B cell maturation, proliferation, and positive selection in the FDC zone of murine splenic germinal centers. Immunity 22:749-61
Carter, Robert H (2004) B cells: new ways to inhibit their function in rheumatoid arthritis. Curr Rheumatol Rep 6:357-63
Brooks, Stephen R; Kirkham, Perry M; Freeberg, Larry et al. (2004) Binding of cytoplasmic proteins to the CD19 intracellular domain is high affinity, competitive, and multimeric. J Immunol 172:7556-64
Cherukuri, Anu; Shoham, Tsipi; Sohn, Hae Won et al. (2004) The tetraspanin CD81 is necessary for partitioning of coligated CD19/CD21-B cell antigen receptor complexes into signaling-active lipid rafts. J Immunol 172:370-80
Brooks, S R; Li, X; Volanakis, E J et al. (2000) Systematic analysis of the role of CD19 cytoplasmic tyrosines in enhancement of activation in Daudi human B cells: clustering of phospholipase C and Vav and of Grb2 and Sos with different CD19 tyrosines. J Immunol 164:3123-31
Li, X; Carter, R H (2000) CD19 signal transduction in normal human B cells: linkage to downstream pathways requires phosphatidylinositol 3-kinase, protein kinase C and Ca2+. Eur J Immunol 30:1576-86