Literature DB >> 8823302

Heterogeneity and clinical significance of glomerular-binding antibodies in systemic lupus erythematosus.

J B Lefkowith1, M Kiehl, J Rubenstein, R DiValerio, K Bernstein, L Kahl, R L Rubin, M Gourley.   

Abstract

We used an ELISA employing extracts of human glomerular basement membrane (GBM) to detect, characterize, and evaluate the clinical significance of glomerular-binding IgG in patients with SLE nephritis. Most patients with SLE nephritis exhibited GBM-binding IgG, although many patients with active nonrenal SLE or symptomatic, drug-induced lupus had similar reactivity, albeit at lower levels. IgG binding to GBM in SLE nephritis patients was decreased by DNase pretreatment of GBM, restored after DNase with nuclear antigens (most notably with nucleosomes), inhibited by exogenous nuclear antigens (particularly nucleosomes), but unaffected by exposure of serum to DNase/high ionic strength. The characteristics of IgG binding to GBM largely paralleled the patients' underlying autoimmune response, which was dominated either by antibodies to DNA/nucleosomes or to nucleosomes alone. Binding of lupus sera to nonrenal extracellular matrix (even with nucleosomes) was not equivalent to GBM. Collagenase pretreatment of GBM variably decreased IgG binding, depending on the level and type of binding. SLE nephritis patients with high levels of GBM-binding IgG exhibited more severe disease clinically, but the same renal histopathology, as patients with lower levels. The level of GBM-binding IgG at presentation did not predict the therapeutic response, but decreased in responders to therapy. In sum, glomerular-binding IgG in lupus nephritis binds to epitopes on chromatin, which adheres to GBM in part via collagen. These autoantibodies appear necessary, but not sufficient, for the development of nephritis, and correlate with clinical rather than histopathologic parameters of disease activity.

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Year:  1996        PMID: 8823302      PMCID: PMC507563          DOI: 10.1172/JCI118924

Source DB:  PubMed          Journal:  J Clin Invest        ISSN: 0021-9738            Impact factor:   14.808


  46 in total

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2.  Subnucleosome structures as substrates in enzyme-linked immunosorbent assays.

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Review 3.  Nephritogenic autoantibodies in lupus: current concepts and continuing controversies.

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Review 4.  Basement membrane proteins: structure, assembly, and cellular interactions.

Authors:  M Paulsson
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5.  Cross-reactive binding patterns of monoclonal antibodies to DNA are often caused by DNA/anti-DNA immune complexes.

Authors:  K Brinkman; R M Termaat; J de Jong; H G van den Brink; J H Berden; R J Smeenk
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6.  Anti-DNA antibodies bind directly to renal antigens and induce kidney dysfunction in the isolated perfused rat kidney.

Authors:  E Raz; M Brezis; E Rosenmann; D Eilat
Journal:  J Immunol       Date:  1989-05-01       Impact factor: 5.422

7.  Immunogenic DNA-related factors. Nucleosomes spontaneously released from normal murine lymphoid cells stimulate proliferation and immunoglobulin synthesis of normal mouse lymphocytes.

Authors:  D A Bell; B Morrison; P VandenBygaart
Journal:  J Clin Invest       Date:  1990-05       Impact factor: 14.808

8.  Autoantibodies associated with lupus induced by diverse drugs target a similar epitope in the (H2A-H2B)-DNA complex.

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Journal:  Kidney Int       Date:  1992-06       Impact factor: 10.612

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4.  Autoimmunity caused by disruption of central T cell tolerance. A murine model of drug-induced lupus.

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8.  Pharmacodynamics of recombinant human DNase I in serum.

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9.  Isolation of anti-nucleosome antibodies from the plasma of lupus nephritis patients.

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