DOI: 10.4049/jimmunol.140.2.354. In vivo obtained antigen presented by germinal center B cells to T cells in vitro.

In vivo obtained antigen presented by germinal center B cells to T cells in vitro.

10.4049/jimmunol.140.2.354

Crossref journal-article

Oxford University Press (OUP)

The Journal of Immunology (286)

Abstract

Abstract Shortly after secondary immunization germinal center (GC) B cells obtain antigen from follicular dendritic cells (FDC) in the form of immune complexes. This antigen appears to be degraded by the GC B cells and may be processed for presentation to T cells. The present study was undertaken to determine whether GC B cells can process and present antigen obtained from FDC in vivo to appropriate T cells in vitro. GC B cells were isolated from immune mice with the use of Percoll density separation followed by a panning procedure which utilizes the ability of the plant lectin, peanut agglutinin (PNA), to selectively bind to GC B cells. The enriched GC B cells were approximately 80% highly positive for PNA, 97% positive for Ia and surface IgM, but less than 0.01% positive for Thy-1.2 or esterase. In some experiments, this population was further purified to near 100% highly PNA-positive cells with the use of fluoresceinated PNA and a fluorescence-activated cell sorter. Cell sorting analysis indicated that the antigen (125I-labeled ovalbumin (OVA)) was restricted to the highly PNA-positive cell fraction. The capacity of these highly PNA-positive B cells to present antigen was assessed by monitoring interleukin 2 (IL-2) production by the OVA-specific T cell hybridoma, 3DO-54.8. GC B cells obtained from mice 3 wk or more after secondary immunization did not elicit IL-2 production in the absence of added OVA. However, GC B cells isolated as early as 1 day and for over 1 wk after a challenge with OVA, were able to stimulate high levels of IL-2 production, in the absence of adding OVA to the cell cultures. This response was maximal on day 5 and corresponded precisely with the kinetics of the ultrastructural studies which document the uptake of antigen by GC B cells in vivo. The FDC-derived antigen was remarkably immunogenic when compared with exogenous antigen. These findings demonstrated that antigen obtained in vivo by GC B cells could be processed and presented to T cells. In vivo, GC B cells may induce the T cell help needed for the germinal center reaction, generate B memory cells, and help induce the high titers of antibody associated with the secondary antibody response.

Bibliography

Kosco, M. H., Szakal, A. K., & Tew, J. G. (1988). In vivo obtained antigen presented by germinal center B cells to T cells in vitro. The Journal of Immunology, 140(2), 354â360.

Authors 3

M H Kosco (first)
A K Szakal (additional)
J G Tew (additional)

References 0 Referenced 91

None

Dates

Type	When
Created	2 years, 8 months ago (Dec. 31, 2022, 12:51 a.m.)
Deposited	8 months ago (Jan. 2, 2025, 1:11 p.m.)
Indexed	2 weeks, 3 days ago (Aug. 19, 2025, 6:33 a.m.)
Issued	37 years, 7 months ago (Jan. 15, 1988)
Published	37 years, 7 months ago (Jan. 15, 1988)
Published Print	37 years, 7 months ago (Jan. 15, 1988)

Funders 0

None

BibTeX

@article{Kosco_1988, title={In vivo obtained antigen presented by germinal center B cells to T cells in vitro.}, volume={140}, ISSN={1550-6606}, url={http://dx.doi.org/10.4049/jimmunol.140.2.354}, DOI={10.4049/jimmunol.140.2.354}, number={2}, journal={The Journal of Immunology}, publisher={Oxford University Press (OUP)}, author={Kosco, M H and Szakal, A K and Tew, J G}, year={1988}, month=jan, pages={354–360} }

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