Abstract
We have previously studied B cells, from people and mice, that express rotavirus-specific surface immunoglobulin (RV-sIg) by flow cytometry with recombinant virus-like particles that contain green fluorescent protein. In the present study we characterized circulating B cells with RV-sIg in children with acute and convalescent infection. During acute infection, circulating RV-sIgD- B cells are predominantly large, CD38high, CD27high, CD138+/-, CCR6- α4β7 +, CCR9+, CCR10+, cutaneous lymphocyte antigen-negative (CLA-), L-selectinint/-, and sIgM +, sIgG-, sIgA+/- lymphocytes. This phenotype likely corresponds to gut-targeted plasma cells and plasmablasts. During convalescence the phenotype switches to small and large lymphocytes, CD38 int/-, CD27int/-, CCR6+, α4β7 +/-, CCR9+/- and CCR10-, most likely representing RV-specific memory B cells with both gut and systemic trafficking profiles. Of note, during acute RV infection both total and RV-specific murine IgM and IgA antibody-secreting cells migrate efficiently to CCL28 (the CCR10 ligand) and to a lesser extent to CCL25 (the CCR9 ligand). Our results show that CCR10 and CCR9 can be expressed on IgM as well as IgA antibody-secreting cells in response to acute intestinal infection, likely helping target these cells to the gut. However, these intestinal infection-induced plasmablasts lack the CLA homing receptor for skin, consistent with mechanisms of differential CCR10 participation in skin T versus intestinal plasma cell homing. Interestingly, RV memory cells generally lack CCR9 and CCR10 and instead express CCR6, which may enable recruitment to diverse epithelial sites of inflammation.
| Original language | English |
|---|---|
| Pages (from-to) | 10967-10976 |
| Number of pages | 10 |
| Journal | Journal of Virology |
| Volume | 78 |
| Issue number | 20 |
| DOIs | |
| State | Published - Oct 2004 |
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