CD22 regulates B lymphocyte function in vivo through both ligand-dependent and ligand-independent mechanisms

被引:0
作者
Jonathan C Poe
Yoko Fujimoto
Minoru Hasegawa
Karen M Haas
Ann S Miller
Isaac G Sanford
Cheryl B Bock
Manabu Fujimoto
Thomas F Tedder
机构
[1] Duke University Medical Center,Department of Immunology
[2] Kanazawa University Graduate School of Medical Science,Department of Dermatology
[3] University of Tokyo,Department of Dermatology, Faculty of Medicine
来源
Nature Immunology | 2004年 / 5卷
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摘要
The interaction of CD22 with α2,6-linked sialic acid ligands has been widely proposed to regulate B lymphocyte function and migration. Here, we generated gene-targeted mice that express mutant CD22 molecules that do not interact with these ligands. CD22 ligand binding regulated the expression of cell surface CD22, immunoglobulin M and major histocompatibility complex class II on mature B cells, maintenance of the marginal zone B cell population, optimal B cell antigen receptor–induced proliferation, and B cell turnover rates. However, CD22 negative regulation of calcium mobilization after B cell antigen receptor ligation, CD22 phosphorylation, recruitment of SHP-1 to CD22 and B cell migration did not require CD22 ligand engagement. These observations resolve longstanding questions regarding the physiological importance of CD22 ligand binding in the regulation of B cell function in vivo.
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页码:1078 / 1087
页数:9
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