Engagement of the B lymphocyte antigen receptor induces presentation of intrinsic immunoglobulin peptides on major histocompatibility complex class II molecules

Bartnes, Kristian; Hannestad, Kristian

doi:10.1002/eji.1830270512

Cited by 16 publications

(16 citation statements)

References 46 publications

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“…Finally, peptides from the BCR V region may provide an avenue of T cell help to autoreactive B cells. The BCR V region is promising in this regard because of the enormous diversity encompassed by V region peptides and because such peptides can be self-presented in class II MHC by activated B cells, which presumably are dependent upon T cell help (25)(26)(27)(28)(29)(30)(31)(32)(33)(34). We refer to this potential avenue of help to autoreactive B cells as the receptor presentation hypothesis (35).…”

Section: T Cell Tolerance To Germline-encoded Antibody Sequences In Amentioning

confidence: 99%

T Cell Tolerance to Germline-Encoded Antibody Sequences in a Lupus-Prone Mouse

Guo

Smith

Guth

et al. 2005

The Journal of Immunology

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The BCR V region has been implicated as a potential avenue of T cell help for autoreactive B cells in systemic lupus erythematosus. In principle, either germline-encoded or somatically generated sequences could function as targets of such help. Preceding studies have indicated that class II MHC-restricted T cells in normal mice attain a state tolerance to germline-encoded Ab diversity. In this study, we tested whether this tolerance is intact in systemic lupus erythematosus-prone (New Zealand Black × SWR)F1 mice (SNF1). Using a hybridoma sampling approach, we found that SNF1 T cells were tolerant to germline-encoded Ab sequences. Specifically, they were tolerant to germline-encoded sequences derived from a lupus anti-chromatin Ab that arose spontaneously in this strain. This was true both for diseased and prediseased mice. Thus, there does not appear to be a global defect in T cell tolerance to Ab V regions in this autoimmune-prone strain either before or during autoimmune disease.

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Section: T Cell Tolerance To Germline-encoded Antibody Sequences In Amentioning

confidence: 99%

T Cell Tolerance to Germline-Encoded Antibody Sequences in a Lupus-Prone Mouse

Guo

Smith

Guth

et al. 2005

The Journal of Immunology

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“…Furthermore, constitutive presentation is independent of maturation of APC and intercellular antigen transfer in vitro , as cells that were paraformaldehyde fixed immediately after preparation were stimulatory, and a co‐culture of spleen cells from BALB/c (I‐A d , IgC H a ,) and BXSB (I‐A b , IgC H b ,) failed to stimulate B5 (K. Bartnes, unpublished). Confirming the poor antigenicity of native IgG2a b in vitro , constitutive presentation was weak or absent in specific pathogen‐free (SPF) healthy animals, which had low levels of circulating IgG2a b –C3 complexes and not more than a few hundred µg/ml of serum IgG2a b 13,14 . In contrast, spleen cells from mice reared under less rigorous microbial control regularly elicited strong B5 hybridoma responses, 9,13 demonstrating a profound influence of environmental factors on the constitutive presentation of the IgG2a b self‐antigen.…”

Section: Introductionmentioning

confidence: 93%

“…Notably, the γ2a b 435–451/I‐A d reactive T‐cell hybridoma, B5, responds to APC from IgC H b , I‐A d mice in the absence of exogenous IgG2a b and should represent a useful, quantitative probe for analysing constitutive γ2a b /I‐A d presentation in vivo . Thus, B5 is insensitive to B7‐mediated signals, 14 the interactions of the γ2a b determinant with the B5 antigen receptor and I‐A d have been characterized in detail, 10,15 , 16 and the B5‐defined epitope is among the predominant determinants generated by processing of IgG2a b (refs 10,11; K. Bartnes, unpublished). Furthermore, constitutive presentation is independent of maturation of APC and intercellular antigen transfer in vitro , as cells that were paraformaldehyde fixed immediately after preparation were stimulatory, and a co‐culture of spleen cells from BALB/c (I‐A d , IgC H a ,) and BXSB (I‐A b , IgC H b ,) failed to stimulate B5 (K. Bartnes, unpublished).…”

Section: Introductionmentioning

confidence: 99%

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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“…Many synthetic subunits can be substituted for proteogenic amino acids to impede proteolysis. These include D-amino acids (Bartnes et al, 1997), β-amino acids (Webb et al, 2005), psi-bonded amino acids (Stemmer et al, 1999), and the shifting of the R group by one atom to create poly- N -substituted glycines (peptoids) where the side chains are appended to the nitrogen atom of the peptide backbone (Gocke et al, 2009). …”

Section: Improving T-cell Epitopesmentioning

confidence: 99%

Advances in T-Cell Epitope Engineering

Pentier¹,

Sewell²,

Miles³

2013

Front. Immunol.

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Engagement of the B lymphocyte antigen receptor induces presentation of intrinsic immunoglobulin peptides on major histocompatibility complex class II molecules

Cited by 16 publications

References 46 publications

T Cell Tolerance to Germline-Encoded Antibody Sequences in a Lupus-Prone Mouse

T Cell Tolerance to Germline-Encoded Antibody Sequences in a Lupus-Prone Mouse

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

Advances in T-Cell Epitope Engineering

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Engagement of the B lymphocyte antigen receptor induces presentation of intrinsic immunoglobulin peptides on major histocompatibility complex class II molecules

Cited by 16 publications

References 46 publications

T Cell Tolerance to Germline-Encoded Antibody Sequences in a Lupus-Prone Mouse

T Cell Tolerance to Germline-Encoded Antibody Sequences in a Lupus-Prone Mouse

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

Advances in T-Cell Epitope Engineering

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Product

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