Is rapid proliferation in B centroblasts linked to somatic mutation in memory B cell clones?

Antigen-reactive B cells accumulate mutations in the variable (v) regions of their immunoglobulin genes during certain phases of T cell-dependent (TD) antibody responses. This is associated with a rise in the affinity of specific antibody. The time when somatic mutations are accumulating seems to coincide with the presence of germinal centres. This has led to the suggestion that a mechanism leading to a high rate of base pair substitution in immunoglobulin v region genes might operate in centroblasts in germinal centres. The rate of accumulation of mutations in v region genes is likely to relate to the number of specific B cells in cycle and their rate of cell division. The present report provides evidence pointing to centroblasts having a remarkably short cell cycle time of some 6 to 7 hours. This rapid rate of proliferation may explain the clonal expansion which occurs in the early phase of TD antibody responses and the efficiency with which high affinity mutants are subsequently selected.

[1]  D. Appleton,et al.  THE METAPHASE ARREST TECHNIQUE , 1980, Cell and tissue kinetics.

[2]  J. Yagüe,et al.  The T cell receptor: the α and β chains define idiotype, and antigen and MHC specificity , 1985, Cell.

[3]  D. G. Osmond,et al.  Pre-B cells in mouse bone marrow: immunofluorescence stathmokinetic studies of the proliferation of cytoplasmic mu-chain-bearing cells in normal mice. , 1983, Journal of immunology.

[4]  N. Maizels,et al.  The T-cell-independent immune response to the hapten NP uses a large repertoire of heavy chain genes , 1985, Cell.

[5]  C. Milstein,et al.  Mutation Drift and Repertoire Shift in the Maturation of the Immune Response , 1987, Immunological reviews.

[6]  G. Klaus,et al.  The Follicular Dendritic Cell: Its Role in Antigen Presentation in the Generation of Immunological Memory , 1980, Immunological reviews.

[7]  D. Gray,et al.  Antigen‐Driven Selection of Virgin and Memory B Cells , 1986, Immunological reviews.

[8]  G. Thorbecke,et al.  Relationship of germinal centers in lymphoid tissue to immunologic memory. VI. Transfer of B cell memory with lymph node cells fractionated according to their receptors for peanut agglutinin. , 1983, Journal of immunology.

[9]  D. Gray,et al.  Selective depression of thymus-independent anti-DNP antibody responses induced by adult but not neonatal splenectomy. , 1985, Clinical and experimental immunology.

[10]  D. Gray,et al.  Differences in the recruitment of virgin B cells into antibody responses to thymus‐dependent and thymus‐independent type‐2 antigens , 1986, European journal of immunology.

[11]  S. Tonegawa Somatic generation of antibody diversity , 1983, Nature.

[12]  D. Gray,et al.  Virgin B cell recruitment and the lifespan of memory clones during antibody responses to 2,4‐dinitrophenyl‐hemocyanin , 1986, European journal of immunology.

[13]  K. Rajewsky,et al.  Somatic mutation and clonal expansion of B cells in an antigen‐driven immune response. , 1985, The EMBO journal.