Abstract

The long term goal of this proposal is to gain insight into the cellular and molecular mechanisms underlying the generation of the specific high affinity autoantibodies to self antigens in patients with systemic autoimmune diseases. The B cell repertoire in these patients differ from that in healthy subjects with respect to the specificities of the autoantibodies produced and the phenotype and regulation of the producing cells. Owing to the high level of circulating antibodies binding self and foreign antigens,it has been proposed that in systemic autoimmune diseases the autoantibody response results from a process of polyclonal B cell activation. Our preliminary experiments suggested that in healthy subjects """"""""autoantibodies"""""""" with such functional features can be produced by CD5+B lymphocytes, a discrete subset of the B cell repertoire. These """"""""autoantibodies"""""""" are, mainly, IgM and bind a variety of antigens (polyreactive antibodies). The polyreactivity and low to moderate affinity of the specific monoclonal antibodies, in general IgG, produced by (CD5-) B cells we isolated from vaccinated subjects, and those of the monoclonal specific autoantibodies produced by B cells we isolated from autoimmune patients. We hypothesize that the production of high affinity autoantibodies in patients with systemic autoimmunity results from a process of specific B cell clonal selection and somatic point mutation driven by antigen. To test this hypothesis, we propose to study the contribution of CD5+ and CD%-B cells as well as the CD5-""""""""sister"""""""" B cells we recently identified to the production of specific, possibly, pathogenic (rheumatoid factors and anti-DNA) autoantibodies in patients with systemic autoimmunity (rheumatoid arthritis and systemic lupus erythematosus, respectively), and to clone and sequence the variable gene segments utilized in these autoantibodies. Such cellular and molecular features will be compared with those we recently derived from the study of the high affinity antibody responses elicited by rabies virus and tetanus toxoid vaccines in normal humans. The proposed experiments should yield important information on the role of various B cell subsets, and variable antibody genes in shaping the profile of the human B cell repertoire. In addition, they should provide us with a variety of monoclonal antibody and gene tools essential to approach a systematic probing of the human B cell repertoire.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR040908-02
Application #
3161375
Study Section
Immunological Sciences Study Section (IMS)
Project Start
1992-02-01
Project End
1995-12-31
Budget Start
1993-01-01
Budget End
1993-12-31
Support Year
2
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
New York University
Department
Type
Schools of Medicine
DUNS #
004514360
City
New York
State
NY
Country
United States
Zip Code
10012

  Publications

Zan, Hong; Zhang, Jinsong; Al-Qahtani, Ahmed et al. (2011) Endonuclease G plays a role in immunoglobulin class switch DNA recombination by introducing double-strand breaks in switch regions. Mol Immunol 48:610-22
Xu, Zhenming; Fulop, Zsolt; Wu, Guikai et al. (2010) 14-3-3 adaptor proteins recruit AID to 5'-AGCT-3'-rich switch regions for class switch recombination. Nat Struct Mol Biol 17:1124-35
Zan, Hong; Casali, Paolo (2008) AID- and Ung-dependent generation of staggered double-strand DNA breaks in immunoglobulin class switch DNA recombination: a post-cleavage role for AID. Mol Immunol 46:45-61
Atassi, M Zouhair; Casali, Paolo (2008) Molecular mechanisms of autoimmunity. Autoimmunity 41:123-32
Xu, Zhenming; Pone, Egest J; Al-Qahtani, Ahmed et al. (2007) Regulation of aicda expression and AID activity: relevance to somatic hypermutation and class switch DNA recombination. Crit Rev Immunol 27:367-97
Duquerroy, Stephane; Stura, Enrico A; Bressanelli, Stephane et al. (2007) Crystal structure of a human autoimmune complex between IgM rheumatoid factor RF61 and IgG1 Fc reveals a novel epitope and evidence for affinity maturation. J Mol Biol 368:1321-31
Xu, Zhenming; Zan, Hong; Pal, Zsuzsanna et al. (2007) DNA replication to aid somatic hypermutation. Adv Exp Med Biol 596:111-27
Wu, Xiaoping; Tsai, Connie Y; Patam, Marienida B et al. (2006) A role for the MutL mismatch repair Mlh3 protein in immunoglobulin class switch DNA recombination and somatic hypermutation. J Immunol 176:5426-37
Casali, Paolo; Pal, Zsuzsanna; Xu, Zhenming et al. (2006) DNA repair in antibody somatic hypermutation. Trends Immunol 27:313-21
Komori, Atsumasa; Xu, Zhenming; Wu, Xiaoping et al. (2006) Biased dA/dT somatic hypermutation as regulated by the heavy chain intronic iEmu enhancer and 3'Ealpha enhancers in human lymphoblastoid B cells. Mol Immunol 43:1817-26

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