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Literature DB >> 18310318

Editing and escape from editing in anti-DNA B cells.

Salar N Khan¹, Esther J Witsch, Noah G Goodman, Anil K Panigrahi, Ching Chen, Yufei Jiang, Amy M Cline, Jan Erikson, Martin Weigert, Eline T Luning Prak, Marko Radic.

Abstract

Tolerance to dsDNA is achieved through editing of Ig receptors that react with dsDNA. Nevertheless, some B cells with anti-dsDNA receptors escape editing and migrate to the spleen. Certain anti-dsDNA B cells that are recovered as hybridomas from the spleens of anti-dsDNA H chain transgenic mice also bind an additional, Golgi-associated antigen. B cells that bind this antigen accumulate intracellular IgM. The intracellular accumulation of IgM is incomplete, because IgM clusters are observed at the cell surface. In the spleen, B cells that express the heavy and light chains encoding this IgM are surface IgM-bright and acquire the CD21-high/CD23-low phenotype of marginal zone B cells. Our data imply that expression of an Ig that binds dsDNA and an additional antigen expressed in the secretory compartment renders B cells resistant to central tolerance. In the periphery, these B cells may be sequestered in the splenic marginal zone.

Entities: Gene Species

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Year: 2008 PMID： 18310318 PMCID： PMC2268806 DOI： 10.1073/pnas.0800025105

Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN： 0027-8424 Impact factor: 11.205

39 in total

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6. Editors and editing of anti-DNA receptors.

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8. Autoreactive B cells in the marginal zone that express dual receptors.

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9. Igkappa allelic inclusion is a consequence of receptor editing.

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10. Secondary heavy chain rearrangement: a mechanism for generating anti-double-stranded DNA B cells.

Authors: Debora R Sekiguchi; Robert A Eisenberg; Martin Weigert
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16 in total

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