Monovalent ligation of the B cell receptor induces receptor activation but fails to promote antigen presentation

YM Kim, JYJ Pan, GA Korbel, Victor Peperzak, M Boes, HL Ploegh*

*Corresponding author for this work

Research output: Contribution to journalArticleAcademicpeer-review

Abstract

We explored the role of antigen valency in B cell receptor (BCR) activation and rearrangement of intracellular MHC class 11 compartments as factors that contribute to the efficacy of antigen presentation. Using primary B cells that express a hen egg lysozyme (HEL)-specific BCR, we found that oligomeric HEL more efficiently promoted both BCR activation and internalization than did monovalent HEL, although monovalent HEL, unlike monovalent Fab fragments of anti-Ig, readily triggered the BCR. Nonetheless, oligovalent ligation positions the BCR in a membrane microdomain that is distinct from one engaged in the course of monovalent ligation, as judged by detergent extraction of the BCR. Furthermore, oligovalent HEL induced more pronounced rearrangement of MHC class II-containing antigen-processing compartments. Using videomicroscopy we observed in real time the rearrangement of MHC class 11 compartments as well as delivery of antigen in primary 6 cells. The observed increase in rearrangement of MHC class II-positive compartments and the disposition of antigen-bound BCRs therein correlates with improved presentation of a HEL-clerived epitope. Although monomeric HEL efficiently engages the BCR, presentation of HEL-derived epitopes is impaired compared to oligovalent antigens. This trait may help explain the known ability of soluble, disaggregated antigen to induce a state of B cell tolerance.

Original languageEnglish
Pages (from-to)3327-3332
Number of pages6
JournalProceedings of the National Academy of Sciences of the United States of America
Volume103
Issue number9
DOIs
Publication statusPublished - 28 Feb 2006
Externally publishedYes

Keywords

  • antigen valency
  • MHC class II
  • MHC CLASS-II
  • LIPID RAFTS
  • T-CELL
  • CUTTING EDGE
  • LYMPHOCYTES
  • BCR
  • INTERNALIZATION
  • INDUCTION
  • CLATHRIN
  • PROTEIN

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