Abstract

The immature B cell represents an important window in B lymphocyte development, for it is at this stage that cells expressing B cell antigen receptors (BCRs) specific for endogenous or """"""""self antigens can be identified and eliminated, inactivated, or undergo alterations in their receptor specificity, in processes collectively referred to as B cell tolerance. The long-term objective of this project is to define the molecular basis for differences in the responsiveness of immature and follicular mature B cells to BCR signaling. Although multiple mechanisms of tolerance affect the ultimate fate of the B cell, we have determined that intrinsic or """"""""hard-wired"""""""" differences in BCR-induced signal transduction dictate B cell fate decisions, specifically when isolated from specific sources of B cell extrinsic signals that both immature B cells from the bone marrow and transitional immature B cells from the periphery undergo an abortive entry into the cell cycle followed by apoptosis while mature B cells are induced to proliferate following BCR engagement. Transitional B cells fail to sustain BCR triggered pathways linked to survival, proliferation, and cytoskeletal re-organization and maintain lower levels of unesterified cholesterol in their plasma membrane relative to mature B cells. We have recently shown that this latter phenotype accounts for their inability to localize their BCR into cholesterol-enriched membrane (CEM) compartments following BCR aggregation. As repletion of membrane cholesterol in transitional B cells reverses proximal signaling differences, we hypothesize that developmental differences in cholesterol levels represent the defining difference between immature and mature B cells that dictates their cell fate following BCR engagement. Therefore, we propose to 1) use a genetic approach to specifically upregulate cholesterol biosynthesis in transitional B cells and evaluate potential links between cholesterol content and differential BCR-induced signal transduction and cell fate, 2) use co-crosslinking and genetic systems to determine whether the transient BCR-induced signal transduction in transitional B cells reflects an inability to engage a PIP3-dependent PIP2 regenerating amplification loop and 3) to determine if transient BCR-induced signaling in transitional B cells impacts on """"""""inside-out"""""""" integrin activation. In autoimmune diseases, B lymphocytes that are normally inactive become activated and secrete autoantibodies that contribute to the disease process. We propose to determine if alterations in cholesterol levels can contribute to the activation of these potentially dangerous B lymphocytes and thereby suggest targets for future treatment of B cell-dependent autoimmune diseases. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI032592-15
Application #
7386714
Study Section
Cellular and Molecular Immunology - B Study Section (CMIB)
Program Officer
Nasseri, M Faraz
Project Start
1993-05-01
Project End
2012-04-30
Budget Start
2008-05-01
Budget End
2009-04-30
Support Year
15
Fiscal Year
2008
Total Cost
$367,321
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Pathology
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Kobayashi, Takashi; Kim, Tae Soo; Jacob, Anand et al. (2009) TRAF6 is required for generation of the B-1a B cell compartment as well as T cell-dependent and -independent humoral immune responses. PLoS One 4:e4736
Stadanlick, Jason E; Kaileh, Mary; Karnell, Fredrick G et al. (2008) Tonic B cell antigen receptor signals supply an NF-kappaB substrate for prosurvival BLyS signaling. Nat Immunol 9:1379-87
Brezski, Randall J; Monroe, John G (2007) B cell antigen receptor-induced Rac1 activation and Rac1-dependent spreading are impaired in transitional immature B cells due to levels of membrane cholesterol. J Immunol 179:4464-72
Grande, S M; Katz, E; Crowley, J E et al. (2006) Cellular ITAM-containing proteins are oncoproteins in nonhematopoietic cells. Oncogene 25:2748-57
Karnell, Fredrick G; Brezski, Randall J; King, Leslie B et al. (2005) Membrane cholesterol content accounts for developmental differences in surface B cell receptor compartmentalization and signaling. J Biol Chem 280:25621-8
Skalet, Alison H; Isler, Jennifer A; King, Leslie B et al. (2005) Rapid B cell receptor-induced unfolded protein response in nonsecretory B cells correlates with pro- versus antiapoptotic cell fate. J Biol Chem 280:39762-71
Fuentes-Panana, Ezequiel M; Bannish, Gregory; van der Voort, Dustin et al. (2005) Ig alpha/Ig beta complexes generate signals for B cell development independent of selective plasma membrane compartmentalization. J Immunol 174:1245-52
Chung, James B; Wells, Andrew D; Adler, Scott et al. (2003) Incomplete activation of CD4 T cells by antigen-presenting transitional immature B cells: implications for peripheral B and T cell responsiveness. J Immunol 171:1758-67
Chung, James B; Sater, Richard A; Fields, Michele L et al. (2002) CD23 defines two distinct subsets of immature B cells which differ in their responses to T cell help signals. Int Immunol 14:157-66
Chiang, M Y; Monroe, J G (2001) Role for transcription Pax5A factor in maintaining commitment to the B cell lineage by selective inhibition of granulocyte-macrophage colony-stimulating factor receptor expression. J Immunol 166:6091-8

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