The regulation of IgA class switching

The regulation of IgA class switching

Key Points IgA is the most abundant isotype antibody in the intestinal mucosa, where it provides a first line of immune protection against commensal, ingested and sexually transmitted agents. IgA uses a high-affinity binding system to neutralize toxins and pathogens and a low-affinity binding system...

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Veröffentlicht in:Nature reviews. Immunology 2008-06, Vol.8 (6), p.421-434
1. Verfasser: Cerutti, Andrea
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Antibodies
Antigens
Bacteria
Biomedical and Life Sciences
Biomedicine
Bone marrow
Dendritic cells
Gene expression
Gene Expression Regulation - immunology
Gene mutations
Genes
Health aspects
Humans
Immune system
Immunity, Mucosal - genetics
Immunoglobulin A
Immunoglobulin A - biosynthesis
Immunoglobulin A - blood
Immunoglobulin A - genetics
Immunoglobulin Class Switching - genetics
Immunoglobulins
Immunology
Kinases
Microorganisms
Proteins
review-article
Vaccines
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Zusammenfassung:Key Points IgA is the most abundant isotype antibody in the intestinal mucosa, where it provides a first line of immune protection against commensal, ingested and sexually transmitted agents. IgA uses a high-affinity binding system to neutralize toxins and pathogens and a low-affinity binding system to confine commensal bacteria to the intestinal lumen. B cells acquire the capability to produce IgA by undergoing class-switch recombination (CSR), a process that requires germline transcription of the heavy chain constant α gene (C α ) and expression of activation-induced cytidine deaminase (AID), an essential component of the CSR machinery. Together with post-IgA CSR modifications, IgA CSR generates multiple molecular forms of IgA proteins, each endowed with distinct topography and functions. In vivo and in vitro studies show that B cells undergo IgA class switching through both T-cell-dependent and T-cell-independent pathways, which generate high- and low-affinity IgA antibodies, respectively. T-cell-dependent IgA class switching requires T-cell help to B cells via CD40 ligand (CD40L) and the cytokine transforming growth factor-β1 (TGFβ1), whereas T-cell-independent IgA class switching involves innate signals provided by microbial Toll-like receptor (TLR) ligands and CD40L-related dendritic cell (DC) mediators, including B-cell-activating factor (BAFF) and a proliferation-inducing ligand (APRIL). TGFβ1 induces germline C α gene transcription through SMAD (mothers against decapentaplegic) proteins, whereas CD40L triggers AID expression through nuclear factor-κB (NF-κB). BAFF and APRIL activate B cells by engaging transmembrane activator and calcium-modulating cyclophilin-ligand interactor (TACI), a receptor that triggers AID expression via NF-κB and germline C α gene transcription through a signalling pathway that remains poorly understood. In the gut, T-cell-dependent IgA class switching takes place in the germinal centres of organized lymphoid structures, including Peyer's patches, whereas T-cell-independent IgA class switching occurs in the non-organized lymphoid tissue of the lamina propria. Nitric oxide from a subset of mucosal DCs enhances T-cell-dependent IgA class switching by upregulating the expression of TGFβ1 receptor on B cells, and T-cell-independent IgA class switching by augmenting the production of BAFF and APRIL by DCs. Intestinal epithelial cells produce APRIL and thymic stromal lymphopoietin (TSLP), a DC-activating cytokine with APRIL-ind
ISSN:1474-1733
1474-1741
DOI:10.1038/nri2322