Rotavirus-Specific CD5+ B Cells in Young Children Exhibit a Distinct Antibody Repertoire Compared with CD5− B Cells
pmid: 16698423
Rotavirus-Specific CD5+ B Cells in Young Children Exhibit a Distinct Antibody Repertoire Compared with CD5− B Cells
Antiviral antibody responses in infants are limited in quality. One reason for this finding could be that the majority of B cells in infants are CD5+ cells, a subset of B cells that is thought to contain cells expressing polyreactive, low-affinity B cell receptors. We analyzed the rotavirus (RV)-specific antibody heavy chain variable region (VH) repertoire in CD5+ and CD5- B cells of four RV-infected children between 10 and 19 months of age. We found that the RV-specific B cell repertoire in CD5+ cells was VH3 family biased, in contrast to the VH1/VH4 dominance seen in CD5- B cells. The immunodominant RV-specific gene segment in CD5- B cells was VH1-46, which is the dominant segment used in RV-specific peripheral blood B cells from infants and adults. In contrast, the immunodominant gene segment was VH3-23 in RV-specific CD5+ B cells, which is the dominant gene segment in randomly selected B cells. Both RV-specific CD5+ and RV-specific CD5- B cells from all children studied demonstrated very low frequencies of somatic mutations. In conclusion, CD5+ B cells in infants responding to RV use an antibody gene repertoire that differs from the virus-specific repertoire of CD5- B cells, and both CD5+ and CD5- RV-specific B cells exhibit a low frequency of somatic mutations.
- Vanderbilt University Medical Center United States
- Monroe Carell Jr. Children's Hospital United States
- Vanderbilt University United States
Male, Rotavirus, Base Sequence, Molecular Sequence Data, B-Lymphocyte Subsets, Immunoglobulin Variable Region, Infant, Antibodies, Viral, CD5 Antigens, Complementarity Determining Regions, Rotavirus Infections, Antibody Formation, Mutation, Humans, Female, Immunoglobulin Heavy Chains
Male, Rotavirus, Base Sequence, Molecular Sequence Data, B-Lymphocyte Subsets, Immunoglobulin Variable Region, Infant, Antibodies, Viral, CD5 Antigens, Complementarity Determining Regions, Rotavirus Infections, Antibody Formation, Mutation, Humans, Female, Immunoglobulin Heavy Chains
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