Abstract

The murine CD21/Cr2 gene encodes two proteins demonstrated to be critical in the acquisition of an optimal immune response. Long considered as a phagocytic receptor for Complement-bearing immune complexes, the CD21 pathway now includes signals for B-cell survival and optimal activation, and presentation of native antigen by follicular dendritic cells (FDC) in the germinal centers of the spleen. The expression of murine CD21 is tightly controlled. The proteins are only found on B-cells during a specific stage of differentiation, and are expressed by FDC once these cells have taken up their position within the spleen. This competing application proposes to continue the laboratories analysis of the mechanism of CD21 gene control, and to initiate a new project to dissect the transcriptional pathways that are activated (or inactivated) upon receptor ligation. We propose that the transcription of the CD21 gene is regulated by a set of transcription factors that are present in all lymphocytes and that the lack of expression by T-cells is due to either (1) the presence of a site specific, T-cell specific histone deacetylase, or (2) a site specific, B-cell specific histone acetylase. Published and preliminary data supports DNA accessibility as a primary determinant of CD21 expression in lymphocytes. In vivohomologous recombination experiments are proposed to dissect the role of key regulatory sites in the control of CD21 expression during B-cell differentiation and by FDC. The second major hypothesis to be tested is that B-cell activation via CD21 ligation, plus or minus surface Ig activation, leads to a pathway of transcriptional control that directly influences the state of B-cell differentiation and activation. Using novel gene analysis approaches, we propose to fully characterize these transcriptional pathways for the expression (depression) of known and novel genes. Elucidation of these pathways will lead to means by such activation can be minimized when inappropriate, or accentuated when required for the generation of an optimal B-cell response.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI024158-18
Application #
6845265
Study Section
Special Emphasis Panel (ZRG1-IMB (02))
Program Officer
Sawyer, Richard T
Project Start
1986-12-01
Project End
2007-06-30
Budget Start
2005-02-01
Budget End
2007-06-30
Support Year
18
Fiscal Year
2005
Total Cost
$300,000
Indirect Cost

  Institution

Name
University of Utah
Department
Pathology
Type
Schools of Medicine
DUNS #
009095365
City
Salt Lake City
State
UT
Country
United States
Zip Code
84112

  Publications

Donius, Luke R; Weis, Janis J; Weis, John H (2014) Murine complement receptor 1 is required for germinal center B cell maintenance but not initiation. Immunobiology 219:440-9
Donius, Luke R; Orlando, Christopher M; Weis, Janis J et al. (2014) Generation of a novel Cr2 gene allele by homologous recombination that abrogates production of Cr2 but is sufficient for expression of Cr1. Immunobiology 219:53-63
Pioli, Peter D; Debnath, Irina; Weis, Janis J et al. (2014) Zfp318 regulates IgD expression by abrogating transcription termination within the Ighm/Ighd locus. J Immunol 193:2546-53
Pioli, Peter D; Weis, John H (2014) Snail transcription factors in hematopoietic cell development: a model of functional redundancy. Exp Hematol 42:425-30
Debnath, Irina; Roundy, Kirstin M; Pioli, Peter D et al. (2013) Bone marrow-induced Mef2c deficiency delays B-cell development and alters the expression of key B-cell regulatory proteins. Int Immunol 25:99-115
Pioli, Peter D; Dahlem, Timothy J; Weis, Janis J et al. (2013) Deletion of Snai2 and Snai3 results in impaired physical development compounded by lymphocyte deficiency. PLoS One 8:e69216
Donius, Luke R; Handy, Jennifer M; Weis, Janis J et al. (2013) Optimal germinal center B cell activation and T-dependent antibody responses require expression of the mouse complement receptor Cr1. J Immunol 191:434-47
Lochhead, Robert B; Sonderegger, F Lynn; Ma, Ying et al. (2012) Endothelial cells and fibroblasts amplify the arthritogenic type I IFN response in murine Lyme disease and are major sources of chemokines in Borrelia burgdorferi-infected joint tissue. J Immunol 189:2488-501
Wee, Yin Shen; Roundy, Kirstin M; Weis, Janis J et al. (2012) Interferon-inducible transmembrane proteins of the innate immune response act as membrane organizers by influencing clathrin and v-ATPase localization and function. Innate Immun 18:834-45
Sonderegger, F Lynn; Ma, Ying; Maylor-Hagan, Heather et al. (2012) Localized production of IL-10 suppresses early inflammatory cell infiltration and subsequent development of IFN-?-mediated Lyme arthritis. J Immunol 188:1381-93

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