Abstract

The application proposes to test an implication of our central hypothesis that B-cell expression of CD5 results from activation via sIg cross-linking: If CD5 B-cells are generated by antigen-mediated activation, then autoreactive CD5 B-cells must result from ligation by autoantigen. This is thought to be important because of the role that CD5 B-cells play in generating protective antibodies in fetal/neonatal life, their contribution to """"""""natural autoantibody"""""""" and their possible contribution to pathogenic autoantibodies in lupus-like syndromes. The hypothesis will test whether autoantigen can stimulate B-cells so that they produce autoantibody and express a CD5 + (B-1a) phenotype. Using a transgene system in which B-cells produce antibody specific for H-2K*, the application will determine if CD5 B-cells can arise in vivo or in vitro as the result of binding with autoantigen. We will attempt to define the conditions in which responding cells are deleted or are activated and the biochemical basis for these responses. The application also proposes to explore why the x-linked immune deficiency (xid) mutation that alters Bruton's tyrosine kinase (BTK) blocks production of autoantibodies and the generation of CD5 B-cells, yet permits responses to T-dependent antigens. Preliminary data in this system indicate that xid alters the B-cell response to autoantigen such that potential autoreactive cells are deleted. We will now determine how wild type BTK function functions in the production of antibody and the generation of CD5 B-cells. Two consequences of xid have already been identified, an inability to produce bcl-XL in response to B-cell receptor (BCR)-mediated activation and deficiencies in the nuclear expression of NF-kappa B components, c-rel in particular. Based on these preliminary data, the investigator will test the hypotheses that activation of B-cells induces an inhibition of l-kappa-B synthesis and that normal BTK function is needed to induce this inhibition. To understand the normal function of BTK in B-cells, the application proposes to study the interactions of wild type and mutant BTK with the protein Cbl, and SHIP and the subcellular localization of BTK following activation. To study mutant forms of BTK, the application proposes to exploit a transient tranfection system that the investigators have developed to study primary B-cell activation responses. Alternatively, stable transfection of transformed xid B-cells will be used. BTK loss variants of wild type mature murine B-cells will be created. This will enable them to approach the question as to whether BTK is important solely because it is essential at a critical point in B-cell development or whether it serves important functions in mature B-cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
2R01AI015803-19A1
Application #
2501727
Study Section
Immunobiology Study Section (IMB)
Project Start
1979-05-01
Project End
2002-11-30
Budget Start
1997-12-01
Budget End
1998-11-30
Support Year
19
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Tufts University
Department
Pathology
Type
Schools of Medicine
DUNS #
604483045
City
Boston
State
MA
Country
United States
Zip Code
02111

  Publications

Berland, Robert; Wortis, Henry H (2003) Normal B-1a cell development requires B cell-intrinsic NFATc1 activity. Proc Natl Acad Sci U S A 100:13459-64
Berland, Robert; Wortis, Henry H (2002) Origins and functions of B-1 cells with notes on the role of CD5. Annu Rev Immunol 20:253-300
Jin, Lei; McLean, Paul A; Neel, Benjamin G et al. (2002) Sialic acid binding domains of CD22 are required for negative regulation of B cell receptor signaling. J Exp Med 195:1199-205
Ma, Limei; Wortis, Henry H; Kenter, Amy L (2002) Two new isotype-specific switching activities detected for Ig class switching. J Immunol 168:2835-46
Wortis, H H; Berland, R (2001) Cutting edge commentary: origins of B-1 cells. J Immunol 166:2163-6
Berland, R; Wortis, H H (2000) Role of NFAT in the regulation of B-1 cells. Curr Top Microbiol Immunol 252:131-40
Bajpai, U D; Zhang, K; Teutsch, M et al. (2000) Bruton's tyrosine kinase links the B cell receptor to nuclear factor kappaB activation. J Exp Med 191:1735-44
Doody, G M; Billadeau, D D; Clayton, E et al. (2000) Vav-2 controls NFAT-dependent transcription in B- but not T-lymphocytes. EMBO J 19:6173-84
Novina, C D; Kumar, S; Bajpai, U et al. (1999) Regulation of nuclear localization and transcriptional activity of TFII-I by Bruton's tyrosine kinase. Mol Cell Biol 19:5014-24
Berland, R; Wortis, H H (1998) An NFAT-dependent enhancer is necessary for anti-IgM-mediated induction of murine CD5 expression in primary splenic B cells. J Immunol 161:277-85

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