In situ class switching and differentiation to IgA-producing cells in the gut lamina propria

Abstract

One of the front lines of the immune defence is the gut mucosa, where immunoglobulin-α (IgA) is continuously produced to react with commensal bacteria and dietary antigens. It is generally accepted that, after antigenic stimulation in the Peyer's patches, IgA⁺ lymphoblasts (B220⁺IgA⁺) migrate through the lymph and blood circulation, and eventually home to the lamina propria of the intestine^1,2. Mice that lack activation-induced cytidine deaminase (AID) are defective in class switch recombination (CSR) and somatic hypermutation³. CSR changes the immunoglobulin heavy chain constant region (CH) gene being expressed from Cµ to other CH genes, resulting in a switch of the immunoglobulin isotype from IgM to IgG, IgE or IgA. AID^-/- mice also secrete large amounts of immunoglobulin-µ (IgM) into faeces, and accumulate B220^-IgM⁺ plasma cells as well as B220⁺IgM⁺ cells in the gut. Here we show that lamina propria B220⁺IgA⁺ cells have just completed CSR, as they still express both AID and transcripts from circular DNA that has been ‘looped-out’ during CSR. Lamina propria IgM⁺ B cells seem to be pre-committed to switching to IgA⁺ in vitro as well as in vivo. Culturing lamina propria IgM⁺ B cells together with lamina propria stromal cells enhances preferential switching and differentiation of B cells to IgA⁺ plasma cells. We conclude that IgA⁺ cells in the gut lamina propria are generated in situ from B220⁺IgM⁺ lymphocytes.