Abstract

In the systemic vasculitides, immune complexes and anti-neutrophil cytoplasmic autoantibodies (ANCA) are the two major pathogenic mechanisms for recruitment of neutrophils which play a critical pathogenic role. No longer considered cells with a limited program of effector functions, neutrophils participate actively in intercellular adhesive events, synthesize and release a range of cytokines important for inflammatory cascades, and secrete both degradative enzymes and short-lived inflammatory mediators. This new appreciation for the molecular and cell biology of neutrophils, coupled with new insights into the structural genetics and function of Fcgamma receptors which interact with immune complexes and ANCA so characteristics of systemic vasculitis, highlights the critical importance of understanding the determinants which initiate these cell programs. The molecular complexity of human Fcgamma receptors includes allelic polymorphisms which are functionally distinct. For example, the FcgammaRIIA/LR allele expressed on neutrophils is the only human Fcgamma receptor which recognizes human IgG2 efficiently, --thus establishing the precedent for interaction between the qualitative and quantitative nature of the humoral immune response and defined Fcgamma receptor genotypes. This molecular complexity also includes distinct receptor isoforms which on neutrophils engage different signal transduction pathways. These observations provide (1) a genetic basis for individual differences in patient responses in vasculitis, (2) a framework for understanding how the properties of autoantibodies, -- as immune complexes or as ANCA antibodies, -- interplay with Fcgamma receptors on neutrophils to lead to tissue damage, and (3) a potential strategy for selective modulation of receptor function. We hypothesize (1) that autoantibodies bind Fcgamma receptors and trigger neutrophils, and (2) that Fcgamma receptor-mediated neutrophil triggering is important in initiating neutrophil functions including homo- and heterotypic adhesion, synthesis and release of cytokines (eg, IL-1, 1L- 1ra, IL-8, TNFalpha), and release of both granular enzymes and short- lived inflammatory mediators. Furthermore, we hypothesize that (1) the two different FcgammaR expressed on neutrophils engage different signal transduction pathways, and (2) these pathways are amenable to differential pharmacological modulation. Accordingly, we will characterize the pathways of neutrophil activation by the two different neutrophil FcgammaR (FcgammaRIIIB and FcgammaRIIA) and define the properties of this differential activation at the levels of gene transcription and integrated cell programs; investigate the capacity of cryoglobulin immune complexes and ANCA to preferentially engage these two receptor systems and to be blocked by specific pharmacologic and recombinant molecules; and relate these findings to the expression of FcgammaR alleles and clinical manifestations in two prototypic paradigms of systemic vasculitis: Wegener's granulomatosis with ANCA and cryoglobulinemic leukocytoclastic vasculitis. These studies may identify genetic risk factors for disease predisposition and important new approaches for targeted therapeutics in vasculitis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR042476-02
Application #
2081770
Study Section
General Medicine A Subcommittee 2 (GMA)
Project Start
1994-09-15
Project End
1998-08-31
Budget Start
1995-09-01
Budget End
1996-08-31
Support Year
2
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Hospital for Special Surgery
Department
Type
DUNS #
City
New York
State
NY
Country
United States
Zip Code
10021

  Publications

Li, Xinrui; Wu, Jianming; Ptacek, Travis et al. (2013) Allelic-dependent expression of an activating Fc receptor on B cells enhances humoral immune responses. Sci Transl Med 5:216ra175
Niewold, Timothy B; Kelly, Jennifer A; Kariuki, Silvia N et al. (2012) IRF5 haplotypes demonstrate diverse serological associations which predict serum interferon alpha activity and explain the majority of the genetic association with systemic lupus erythematosus. Ann Rheum Dis 71:463-8
Harley, Isaac T W; Niewold, Timothy B; Stormont, Rebecca M et al. (2010) The role of genetic variation near interferon-kappa in systemic lupus erythematosus. J Biomed Biotechnol 2010:
Kelley, James M; Edberg, Jeffrey C; Kimberly, Robert P (2010) Wegener's granulomatosis: a model of auto-antibodies in mucosal autoimmunity. Clin Immunol 134:104-12
Kelley, James M; Edberg, Jeffrey C; Kimberly, Robert P (2010) Pathways: Strategies for susceptibility genes in SLE. Autoimmun Rev 9:473-6
Li, X; Ptacek, T S; Brown, E E et al. (2009) Fcgamma receptors: structure, function and role as genetic risk factors in SLE. Genes Immun 10:380-9
Gibson, Andrew W; Li, Fu Jun; Wu, Jianming et al. (2009) The FCRL3-169CT promoter single-nucleotide polymorphism, which is associated with systemic lupus erythematosus in a Japanese population, predicts expression of receptor protein on CD19+ B cells. Arthritis Rheum 60:3510-2
Qian, Kun; Xie, Fenglong; Gibson, Andrew W et al. (2008) Functional expression of IgA receptor FcalphaRI on human platelets. J Leukoc Biol 84:1492-500
Ptacek, T; Li, X; Kelley, J M et al. (2008) Copy number variants in genetic susceptibility and severity of systemic lupus erythematosus. Cytogenet Genome Res 123:142-7
Kelly, J A; Kelley, J M; Kaufman, K M et al. (2008) Interferon regulatory factor-5 is genetically associated with systemic lupus erythematosus in African Americans. Genes Immun 9:187-94

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