Abstract

Our overall goal is to understand how the breakdown of normal self- tolerance mechanisms leads to systemic autoimmune disease. Transgenic (Tgic) mouse systems developed by several groups including our own have demonstrated that self-reactive B cells can be regulated by a remarkably diverse set of mechanisms, including deletion, anergy and receptor edition. We have shown that B cells expressing a disease-associated Rheumatoid Factor (RF, anti-IgG2a), autoAb are not subject to any of these known regulatory mechanisms in normal mice, a state termed clonal ignorance. Such ignorant lymphocytes may be the precursors of truly pathogenic autoimmune responses. Thus, autoimmune mice differ from normal mice in regulating autoreactive B cells at stages beyond deletion and anergy of newly developed B cells. There are many Ag receptor dependent stages of B cell development--notably development and maintenance of memory B cells--where regulatory checkpoints could exist but have been little explored. By focusing on these later stages of B cell development, we plan to address the fundamental questions: How do normal mice prevent the development of autoreactive B cell clones, whereas autoimmune mice promote development, and how is this autoimmunity sustained? To address this, we will test two hypothesis. The first is that autoAb-secreting clones arise from low affinity precursors that are not censored by anergy or deletion in normal mice, but in autoimmune-prone mice, these clones undergo Ag-driven affinity maturation and memory B cell differentiation. This will be tested in Aim 1 where we will use our AM14 Tgic system and V region """"""""knockin"""""""" versions of it to compare RF B cell memory development in both normal and autoimmune mice in the presence and absence of autoAg. The second hypothesis, suggested by new data from our high affinity RF Tgic system could explain chronicity. We hypothesize that once autoreactive B cells secrete sufficient autoAb for a given specificity, the autoAg can no longer delete or anergize B cells specific for that autoAg, because the presence of the autoAb removes or block the autoAg. This will be tested in Aim 2 where we will seek direct evidence that a self-amplifying circuit can propagate autoAb production in both Tgic and non-Tgic mice. This work could elucidate a novel mechanism by which autoimmunity, once induced, may be propagate indefinitely, an important feature of human SLE. To determine where B cell regulation fails in systemic autoimmunity is critical, as it would permit molecular studies directed at the cellular mechanism and would provide specific therapeutic targets. This is the ongoing focus of our lab and of this proposal.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI036529-08
Application #
6484677
Study Section
Project Start
2001-09-01
Project End
2002-09-29
Budget Start
Budget End
Support Year
8
Fiscal Year
2001
Total Cost
$247,465
Indirect Cost

  Institution

Name
Yale University
Department
Type
DUNS #
082359691
City
New Haven
State
CT
Country
United States
Zip Code
06520

  Publications

Doyle, Hester A; Mamula, Mark J (2012) Autoantigenesis: the evolution of protein modifications in autoimmune disease. Curr Opin Immunol 24:112-8
Kamanaka, Masahito; Huber, Samuel; Zenewicz, Lauren A et al. (2011) Memory/effector (CD45RB(lo)) CD4 T cells are controlled directly by IL-10 and cause IL-22-dependent intestinal pathology. J Exp Med 208:1027-40
Choi, Je-Min; Shin, Jae-Hun; Sohn, Myung-Hyun et al. (2010) Cell-permeable Foxp3 protein alleviates autoimmune disease associated with inflammatory bowel disease and allergic airway inflammation. Proc Natl Acad Sci U S A 107:18575-80
Sweet, Rebecca A; Christensen, Sean R; Harris, Michelle L et al. (2010) A new site-directed transgenic rheumatoid factor mouse model demonstrates extrafollicular class switch and plasmablast formation. Autoimmunity 43:607-18
Sanjabi, Shomyseh; Zenewicz, Lauren A; Kamanaka, Masahito et al. (2009) Anti-inflammatory and pro-inflammatory roles of TGF-beta, IL-10, and IL-22 in immunity and autoimmunity. Curr Opin Pharmacol 9:447-53
Herlands, Robin A; Christensen, Sean R; Sweet, Rebecca A et al. (2008) T cell-independent and toll-like receptor-dependent antigen-driven activation of autoreactive B cells. Immunity 29:249-60
Shlomchik, Mark J (2008) Sites and stages of autoreactive B cell activation and regulation. Immunity 28:18-28
Christensen, Sean R; Shlomchik, Mark J (2007) Regulation of lupus-related autoantibody production and clinical disease by Toll-like receptors. Semin Immunol 19:11-23
Herlands, Robin A; William, Jacqueline; Hershberg, Uri et al. (2007) Anti-chromatin antibodies drive in vivo antigen-specific activation and somatic hypermutation of rheumatoid factor B cells at extrafollicular sites. Eur J Immunol 37:3339-51
Harvey, Bohdan P; Gee, Renelle J; Haberman, Ann M et al. (2007) Antigen presentation and transfer between B cells and macrophages. Eur J Immunol 37:1739-51

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