New markers for murine memory B cells that define mutated and unmutated subsets

Author:

Anderson Shannon M.1,Tomayko Mary M.2,Ahuja Anupama3,Haberman Ann M.1,Shlomchik Mark J.13

Affiliation:

1. Section of Immunobiology

2. Department of Dermatology, Yale University School of Medicine, New Haven, CT 06510

3. Department of Laboratory Medicine,

Abstract

The study of murine memory B cells has been limited by small cell numbers and the lack of a definitive marker. We have addressed some of these difficulties with hapten-specific transgenic (Tg) mouse models that yield relatively large numbers of antigen-specific memory B cells upon immunization. Using these models, along with a 5-bromo-2′-deoxyuridine (BrdU) pulse-label strategy, we compared memory cells to their naive precursors in a comprehensive flow cytometric survey, thus revealing several new murine memory B cell markers. Most interestingly, memory cells were phenotypically heterogeneous. Particularly surprising was the finding of an unmutated memory B cell subset identified by the expression of CD80 and CD35. We confirmed these findings in an analogous V region knock-in mouse and/or in non-Tg mice. There also was anatomic heterogeneity, with BrdU+ memory cells residing not just in the marginal zone, as had been thought, but also in splenic follicles. These studies impact the current understanding of murine memory B cells by identifying new phenotypes and by challenging assumptions about the location and V region mutation status of memory cells. The apparent heterogeneity in the memory compartment implies either different origins and/or different functions, which we discuss.

Publisher

Rockefeller University Press

Subject

Immunology,Immunology and Allergy

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