Mature B cells class switched to IgD are autoreactive in healthy individuals
Kristi Koelsch, … , J. Donald Capra, Patrick C. Wilson
Kristi Koelsch, … , J. Donald Capra, Patrick C. Wilson
Published June 1, 2007
Citation Information: J Clin Invest. 2007;117(6):1558-1565. https://doi.org/10.1172/JCI27628.
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Research Article Autoimmunity

Mature B cells class switched to IgD are autoreactive in healthy individuals

Abstract

Determination of the origin and fate of autoreactive B cells is critical to understanding and treating autoimmune diseases. We report that, despite being derived from healthy people, antibodies from B cells that have class switched to IgD via genetic recombination (and thus become class switched to Cδ [Cδ-CS] cells) are highly reactive to self antigens. Over half of the antibodies from Cδ-CS B cells bind autoantigens on human epithelioma cell line 2 (HEp-2) cells or antinuclear antigens, and a quarter bind double-stranded DNA; both groups of antibodies are frequently polyreactive. Intriguingly, some Cδ-CS B cells have accumulated basic residues in the antibody variable regions that mediate anti-DNA reactivity via somatic hypermutation and selection, while other Cδ-CS B cells are naturally autoreactive. Though the total percentage was appreciably less than for Cδ-CS cells, a surprising 31% of IgG memory cell antibodies were somewhat autoreactive, and as expected, about 24% of naive cell antibodies were autoreactive. We interpret these findings to indicate either that autoreactive B cells can be induced to class switch to IgD or that autoreactive B cells that use IgD as the B cell receptor are not effectively deleted. Determination of the mechanism by which the majority of Cδ-CS B cells are autoreactive may be important in understanding peripheral tolerance mechanisms and may provide insight into the enigmatic function of the IgD antibody.

Authors

Kristi Koelsch, Nai-Ying Zheng, Qingzhao Zhang, Andrew Duty, Christina Helms, Melissa D. Mathias, Mathew Jared, Kenneth Smith, J. Donald Capra, Patrick C. Wilson

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Figure 5

Cδ-CS can occur for cells that express germline (natural) autoreactive antibodies as well as those that have acquired autoreactivity via somatic mutations.

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Cδ-CS can occur for cells that express germline (natural) autoreactive a...
(A) Cδ-CS antibodies encoded by unmutated (germline) variable genes display levels of HEp-2 autoreactivity, DNA binding, and polyreactivity similar to those from somatically mutated variable genes. Shown are the percentages of antibodies from each subpopulation. (B) Binding curves of 1 μg/ml anti-DNA antibodies from Cδ-CS B cells to DNA were used to calculate absorbencies (blue dots). Comparison of these absorbencies with the frequency of amino acid replacements (red bars) showed that there is no correlation between the affinity for dsDNA and the accumulation of somatic mutations. The variable genes of clones 14 and 17 (asterisks) were reverted to their germline sequences to determine whether the somatic mutations might cause DNA binding. (C) DNA binding is lost when 2 anti-DNA Cδ-CS antibodies (clone 14, blue square; clone 17, blue circle) were expressed from variable genes reverted to the germline unmutated sequences (clone 14, black square; clone 17, black circle). Anti-DNA binding was evaluated by ELISA (absorbance [OD415]) relative to the control 3H9 monoclonal antibody with high affinity for DNA (red line). GL, germline.