The B Cell Receptor Itself Can Activate Complement to Provide the Complement Receptor 1/2 Ligand Required to Enhance B Cell Immune Responses In Vivo

doi:10.1084/jem.20022042

3rd Skeletal Biology and Medicine Symposium

Published 18 August 2003. doi:10.1084/jem.20022042

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© Rockefeller University Press, 0022-1007/2003/8/591 $5.00
The Journal of Experimental Medicine, Volume 198, Number 4, 591-602

The B Cell Receptor Itself Can Activate Complement to Provide the Complement Receptor 1/2 Ligand Required to Enhance B Cell Immune Responses In Vivo

Joerg Rossbacher and Mark J. Shlomchik

Section of Immunobiology and Department of Laboratory Medicine, Yale University School of Medicine, New Haven, CT 06520

Address correspondence to Mark J. Shlomchik, 333 Cedar St., Box 208035, New Haven, CT 06520-8035. Phone: 203-688-2089; Fax: 203-688-2748; email: mark.shlomchik{at}yale.edu

B cells express complement receptors (CRs) that bind activatedfragments of C3 and C4. Immunized CR knockout (KO) mice havelower antibody titers and smaller germinal centers (GCs), demonstratingthe importance of CR signals for the humoral immune response.CR ligands were thought to be generated via complement fixationmediated by preexisting "natural" IgM or early Ab from inefficientlyactivated B cells. This concept was recently challenged by atransgenic (Tg) mouse model that lacks circulating antibodybut still retains membrane IgM (mIgM) and mounts normal immuneresponses. To test whether CR ligands could be generated bythe B cell receptor (BCR) itself, we generated similar micecarrying a mutated mIgM that was defective in C1q binding. Wefound that B cells from such mutant mice do not deposit C3 onB cells upon BCR ligation, in contrast to B cells from mIgMmice. This has implications for the immune response: the mutantmice have smaller GCs than mIgM mice, and they are particularlydeficient in the maintenance of the GC response. These resultsdemonstrate a new BCR-dependent pathway that is sufficient andperhaps necessary to provide a CR1/2 ligand that promotes efficientB cell activation.

Key Words: C1q • IgM • germinal center • CD19 • CD35

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