High-affinity IgM+ memory B cells are defective in differentiation into IgM antibody-secreting cells by re-stimulation with a T cell-dependent antigen

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作者
Yasuyuki Tashiro
Akikazu Murakami
Yasushi Hara
Takeyuki Shimizu
Masato Kubo
Ryo Goitsuka
Hidehiro Kishimoto
Takachika Azuma
机构
[1] Tokyo University of Science,Division of Development and Aging, Research Institute for Biomedical Sciences
[2] Noda,Division of Biosignaling, Research Institute for Biomedical Sciences
[3] Tokyo University of Science,Department of Parasitology & Immunopathoetiology
[4] Noda,Shared equipment room, Research Institute for Biomedical Sciences
[5] Graduate School of Medicine,Department of Immunology
[6] University of the Ryukyus,Division of Molecular Pathology, Research Institute for Biomedical Sciences
[7] Tokyo University of Science,undefined
[8] Noda,undefined
[9] Kochi Medical School,undefined
[10] Kochi University,undefined
[11] Tokyo University of Science,undefined
[12] Noda,undefined
[13] Laboratory for Cytokine Regulation,undefined
[14] Research Center for Integrative Medical Science (IMS),undefined
[15] RIKEN Yokohama Institute,undefined
[16] Antibody Technology Research Center,undefined
[17] Co. Ltd.,undefined
来源
关键词
Memory B-cells (MBCs); Somatic Hypermutation (SHM); Recall Responses; Ab-secreting Cells (ASCs); Plasmablasts;
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摘要
IgM antibodies (Abs) are thought to play a major role in humoral immunity but only at the early stage of the primary immune response. However, two subsets of IgM+ memory B cells (MBCs), one with high affinity gained by means of multiple somatic hypermutation (SHM) and the other with low affinity and no SHMs, are generated through the germinal center (GC)-dependent and GC-independent (non-GC) pathway, respectively, after immunization with (4-hydroxy-3-nitrophenyl)acetyl (NP)-chicken γ-globulin. Surprisingly, an analysis of antibody-secreting cells reveals that a large amount of anti-NP IgM Ab with few SHMs is secreted during the recall response, indicating that only non-GC MBCs have terminal differentiation potential. Since secondary IgM Abs are capable of binding to dinitrophenyl ligands, they likely provide broad cross-reactivity in defense against microbial infection.
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