Literature DB >> 19202057

Sialylated multivalent antigens engage CD22 in trans and inhibit B cell activation.

Adam H Courtney1, Erik B Puffer, Jason K Pontrello, Zhi-Qiang Yang, Laura L Kiessling.   

Abstract

CD22 is an inhibitory coreceptor on the surface of B cells that attenuates B cell antigen receptor (BCR) signaling and, therefore, B cell activation. Elucidating the molecular mechanisms underlying the inhibitory activity of CD22 is complicated by the ubiquity of CD22 ligands. Although antigens can display CD22 ligands, the receptor is known to bind to sialylated glycoproteins on the cell surface. The propinquity of CD22 and cell-surface glycoprotein ligands has led to the conclusion that the inhibitory properties of the receptor are due to cis interactions. Here, we examine the functional consequences of trans interactions by employing sialylated multivalent antigens that can engage both CD22 and the BCR. Exposure of B cells to sialylated antigens results in the inhibition of key steps in BCR signaling. These results reveal that antigens bearing CD22 ligands are powerful suppressors of B cell activation. The ability of sialylated antigens to inhibit BCR signaling through trans CD22 interactions reveals a previously unrecognized role for the Siglec-family of receptors as modulators of immune signaling.

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Year:  2009        PMID: 19202057      PMCID: PMC2650292          DOI: 10.1073/pnas.0807207106

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


  47 in total

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  60 in total

Review 1.  Molecular underpinning of B-cell anergy.

Authors:  Yuval Yarkoni; Andrew Getahun; John C Cambier
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Authors:  Fabian Pfrengle; Matthew S Macauley; Norihito Kawasaki; James C Paulson
Journal:  J Immunol       Date:  2013-07-08       Impact factor: 5.422

Review 5.  Nanoscale materials for probing the biological functions of the glycocalyx.

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Journal:  Glycobiology       Date:  2016-02-24       Impact factor: 4.313

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Authors:  Jennifer Müller; Lars Nitschke
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