作者
Griselda V Zuccarino-Catania, Saheli Sadanand, Florian J Weisel, Mary M Tomayko, Hailong Meng, Steven H Kleinstein, Kim L Good-Jacobson, Mark J Shlomchik
发表日期
2014/7
期刊
Nature immunology
卷号
15
期号
7
页码范围
631-637
出版商
Nature Publishing Group US
简介
Memory B cells (MBCs) are long-lived sources of rapid, isotype-switched secondary antibody-forming cell (AFC) responses. Whether MBCs homogeneously retain the ability to self-renew and terminally differentiate or if these functions are compartmentalized into MBC subsets has remained unclear. It has been suggested that antibody isotype controls MBC differentiation upon restimulation. Here we demonstrate that subcategorizing MBCs on the basis of their expression of CD80 and PD-L2, independently of isotype, identified MBC subsets with distinct functions upon rechallenge. CD80+PD-L2+ MBCs differentiated rapidly into AFCs but did not generate germinal centers (GCs); conversely, CD80PD-L2 MBCs generated few early AFCs but robustly seeded GCs. The gene-expression patterns of the subsets supported both the identity and function of these distinct MBC types. Hence, the differentiation and …
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