Low-level hypermutation in T cell–independent germinal centers compared with high mutation rates associated with T cell–dependent germinal centers

KM Toellner, WE Jenkinson, DR Taylor… - The Journal of …, 2002 - rupress.org
KM Toellner, WE Jenkinson, DR Taylor, M Khan, DMY Sze, DM Sansom, CG Vinuesa
The Journal of experimental medicine, 2002rupress.org
Exceptionally germinal center formation can be induced without T cell help by
polysaccharide-based antigens, but these germinal centers involute by massive B cell
apoptosis at the time centrocyte selection starts. This study investigates whether B cells in
germinal centers induced by the T cell–independent antigen (4-hydroxy-3-nitrophenyl)
acetyl (NP) conjugated to Ficoll undergo hypermutation in their immunoglobulin V region
genes. Positive controls are provided by comparing germinal centers at the same stage of …
Exceptionally germinal center formation can be induced without T cell help by polysaccharide-based antigens, but these germinal centers involute by massive B cell apoptosis at the time centrocyte selection starts. This study investigates whether B cells in germinal centers induced by the T cell–independent antigen (4-hydroxy-3-nitrophenyl)acetyl (NP) conjugated to Ficoll undergo hypermutation in their immunoglobulin V region genes. Positive controls are provided by comparing germinal centers at the same stage of development in carrier-primed mice immunized with a T cell–dependent antigen: NP protein conjugate. False positive results from background germinal centers and false negatives from non-B cells in germinal centers were avoided by transferring B cells with a transgenic B cell receptor into congenic controls not carrying the transgene. By 4 d after immunization, hypermutation was well advanced in the T cell–dependent germinal centers. By contrast, the mutation rate for T cell–independent germinal centers was low, but significantly higher than in NP-specific B cells from nonimmunized transgenic mice. Interestingly, a similar rate of mutation was seen in extrafollicular plasma cells at this stage. It is concluded that efficient activation of hypermutation depends on interaction with T cells, but some hypermutation may be induced without such signals, even outside germinal centers.
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