Induction of long-lived germinal centers associated with persisting antigen after viral infection

被引:166
作者
Bachmann, MF
Odermatt, B
Hengartner, H
Zinkernagel, RM
机构
[1] Inst. for Experimental Immunology, Department of Pathology, University of Zürich, CH-8091 Zürich
[2] Ontario Cancer Institute, Depts. of Med. Biophys. and Immunol., University of Toronto
关键词
D O I
10.1084/jem.183.5.2259
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Vesicular stomatitis virus (VSV) induces an early T cell-independent neutralizing IgM response that is followed by a long-lived, T cell-dependent IgG response. We used the specific amplification factor of several 100X of VSV-virions for immunohistology to analyze the localization of VSV-specific B cells at different time points after immunization. At the peak of the IgM response (day 4), VSV-specific B cells were predominantly present in the red pulp and marginal zone but not in the T area. These B cells were mostly stained in the cytoplasm, characterizing them as antibody secreting cells. By day 6 after immunization, germinal centers (GC) containing surface-stained VSV-specific B cells became detectable and were fully established by day 12. At the same time, large VSV-specific B cell aggregates were present in the red pulp. High numbers of VSV-specific GC associated with persisting antigen were present 1 mo after immunization and later, i.e., considerably longer than has been observed for haptens. Some GC, exhibiting follicular dendritic cells and containing VSV-specific, proliferating B cells were still detectable up to 100 d after immunization Long-lived GC were also observed after immunization with recombinant VSV-glycoprotein in absence of adjuvants. Thus some anti-virally protective (memory) B cells are cycling and locally proliferate in long-lived GC in association with persisting antigen and therefore seem responsible for long-term maintenance of elevated antibody levels. These observations extend earlier studies with carrier hapten antigens in adjuvant depots or complexed with specific IgG; they are the first to show colocalization of antigen and specific memory B cells and to analyze a protective neutralizing antibody response against an acute viral infection.
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页码:2259 / 2269
页数:11
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