Memory B cells isolated from human tonsils are characterized by an activated cell surface phenotype, localization to mucosal epithelium, expression of somatically mutated immunoglobulin (Ig) variable (V) region genes, and a preferential differentiation into plasma cells in vitro. In spleens of both humans and rodents, a subset of memory B cells is believed to reside in the marginal zone of the white pulp. Similar to tonsil-derived memory B cells, splenic marginal zone B cells can be distinguished from naive follicular B cells by a distinct cell surface phenotype and by the presence of somatic mutations in their Ig V region genes. Although differences exist between human naive and memory B cells, no cell surface molecules have been identified that positively identify all memory B cells. In this study, we have examined the expression of the receptor-type protein tyrosine phosphatase CD148 on human B cells. CD148+ B cells present in human spleen exhibited characteristics typical of memory B cells. These included an activated phenotype, localization to the marginal zone, the expression of somatically mutated Ig V region genes, and the preferential differentiation into plasma cells. In contrast, CD148− B cells appeared to be naive B cells due to localization to the mantle zone, the expression of surface antigens typical of unstimulated B cells, and the expression of unmutated Ig V region genes. Interestingly, CD148+ B cells also coexpressed CD27, whereas CD148− B cells were CD27−. These results identify CD148 and CD27 as markers which positively identify memory B cells present in human spleen. Thus, assessing expression of these molecules may be a convenient way to monitor the development of memory B cell responses in immunocompromised individuals or in vaccine trials.
Identification of Functional Human Splenic Memory B Cells by Expression of CD148 and CD27
Address correspondence to Stuart G. Tangye, DNAX Research Institute, 901 California Ave., Palo Alto, CA 94304. Phone: 650-496-1162; Fax: 650-496-1200; E-mail: [email protected]
This paper is dedicated to Bruce F. Bennett, a dear friend and colleague of everyone at DNAX.
DNAX Research Institute is supported by the Schering-Plough Corporation.
G. Aversa and J. de Vries's current address is Novartis Research Institute, Brunner Strasse 59, A-1235 Vienna, Austria.
Stuart G. Tangye, Yong-Jun Liu, Gregorio Aversa, Joseph H. Phillips, Jan E. de Vries; Identification of Functional Human Splenic Memory B Cells by Expression of CD148 and CD27 . J Exp Med 2 November 1998; 188 (9): 1691–1703. doi: https://doi.org/10.1084/jem.188.9.1691
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