X. Li scite author profile

X. Li

2Publications

8Citation Statements Received

141Citation Statements Given

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133

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UiT The Arctic University of Norway

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Antinucleosome Autoantibodies Bind Directly to Cell Lines In Vitro and via the FcγRIIB Receptor to B Lymphocytes In Vivo: A Role for Immune Complexes in Interactions between Antinucleosome IgG2a and B cells of BXSB Lupus Mice

Egorina

Bertelsen

et al. 2004

Scand J Immunol

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The initial novel observation of this study was that most B cells of male BXSB lupus mice bear surface IgG2a b of extrinsic origin. To define the surface antigen, we here examine three (NZBxBXSB)F1-derived IgG2a b monoclonal antibodies (mAbs) selected for binding to cell surfaces. Surprisingly, all three mAbs bound the nucleosome (nuc) particle, the fundamental unit of chromatin and an early target of autoimmunity in systemic lupus erythematosus. Their tentative dissociation constant (K d ) for soluble nuc particles was approximately 7 Â 10The mAbs bound more weakly to both H2A-H2B-DNA and H3-H4-DNA complexes, and in immunoblot they stained all four core histones. The mAbs detected a surface antigen on all cell lines examined, present on viable cells. When stripped of nuc , and in the presence of DNase I, their binding to cell lines improved. Heparin displaced the antigen from the cell surface. In vivo, the three mAbs stained B cells of several BALB/c mice clearly stronger than the isotype control; this differential staining was significantly reduced in FcgRIIBdeficient mice. The results indicate that the three mAbs recognize (a) planted antigen on viable cultured cells and (b) soluble autoantigen in vivo, leading to immune complexes that bind to FcgRIIB. Further experiments demonstrated that antinuc IgG2a could be eluted from splenocytes of a male BXSB lupus mouse. Hence, at least part of the extrinsic IgG2a b found on BXSB B cells may represent FcgRIIB-bound nuc-IgG2a b complexes.

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Genes predisposing to autoimmunity augment constitutive major histocompatibility complex class II‐associated presentation of the self‐antigen IgG2a^bin vivo

Bartnes

Iwamoto

et al. 2000

Immunology

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The self-antigen IgG2ab is poorly presented to a gamma2ab 435-451-reactive I-Ad-restricted T-cell hybridoma unless available in high concentrations or targeted to Fcgamma- or complement receptors. Environmental factors, probably the extent of microbial challenge, profoundly influence the constitutive gamma2ab/I-Ad presentation in IgCHb, H-2d mice. Here we report also a strong genetic impact. Constitutive presentation was highly efficient in spleen and thymus of (NZB x BXSB)F1 mice, which inherit a predisposition to develop lupus. Presentation correlated with disease progression and the serum levels of IgG2ab and IgG2ab complement factor 3 complexes. The finding that constitutive presentation was by far most efficient in males indicated that it was augmented by the Y chromosome-linked autoimmune acceleration Yaa gene. In line with previous data for healthy mice, constitutive gamma2ab/I-Ad presentation was most pronounced in the adherent spleen cell fraction and improved by further enrichment for dendritic cells. Notably, however, whereas in normal mice the gamma2ab determinant was undetectable on B cells lacking surface IgG2ab, such B cells contributed considerably to constitutive presentation in (NZB x BXSB)F1 hybrids. Presumably this resulted from complement receptor-mediated internalization of IgG2ab-containing immune complexes formed in lupus. These data add to the evidence that B cells with self-reactive receptors, known to exist in the mature repertoire, may present non-cognate foreign antigen to anti-foreign helper T lymphocytes and thus differentiate into autoantibody-secreting cells, and might likewise account for the polyclonal B-cell activation characteristic of several autoimmune syndromes.

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X. Li

Antinucleosome Autoantibodies Bind Directly to Cell Lines In Vitro and via the FcγRIIB Receptor to B Lymphocytes In Vivo: A Role for Immune Complexes in Interactions between Antinucleosome IgG2a and B cells of BXSB Lupus Mice

Genes predisposing to autoimmunity augment constitutive major histocompatibility complex class II‐associated presentation of the self‐antigen IgG2a^bin vivo

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X. Li

Antinucleosome Autoantibodies Bind Directly to Cell Lines In Vitro and via the FcγRIIB Receptor to B Lymphocytes In Vivo: A Role for Immune Complexes in Interactions between Antinucleosome IgG2a and B cells of BXSB Lupus Mice

Genes predisposing to autoimmunity augment constitutive major histocompatibility complex class II‐associated presentation of the self‐antigen IgG2abin vivo

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Genes predisposing to autoimmunity augment constitutive major histocompatibility complex class II‐associated presentation of the self‐antigen IgG2a^bin vivo