DOI: 10.4049/jimmunol.129.1.97. Separate signals for human B cell proliferation and differentiation in response to <i>Staphylococcus aureus</i>: evidence for a two-signal model of B cell activation.

Separate signals for human B cell proliferation and differentiation in response to Staphylococcus aureus: evidence for a two-signal model of B cell activation.

10.4049/jimmunol.129.1.97

Crossref journal-article

Oxford University Press (OUP)

The Journal of Immunology (286)

Abstract

Abstract We have investigated the role of T cells in the mitogenic response of human peripheral blood B lymphocytes to killed Cowan strain Staphylococcus aureus (SAC). We found that mononuclear cells exhaustively depleted of T cells by removal of cells rosetting with AET-treated SRBC, or by cytotoxic treatment with the monoclonal antibody anti-Leu-1 and complement, proliferate in response to SAC, but do not differentiate into immunoglobulin- (Ig) secreting cells (ISC). This held true not only for B cells secreting polyclonal Ig detected in a reverse hemolytic plaque-forming cell assay or in ELISA assays for total IgM and IgG, but also for the B cells secreting specific antibody against KLH or tetanus toxoid in response to SAC 2 wk after booster immunization in vivo. We found no evidence for a B cell subset that does not require T help for continued Ig secretion in response to SAC. The differentiative response of B cells to SAC could be restored by the addition of autologous T cells to the T-depleted population. SAC was shown not to stimulate T cells itself; the simultaneous stimulation of T cells with PWM and of B cells with SAC resulted in the ability of very small numbers of T cells to provide the signal required for B cell maturation into ISC. Similarly, supernatants of stimulated T cells efficiently substituted for T cells in this process. Mixed lymphocyte culture supernatants consistently resulted in increased numbers of ISC when added to B cells undergoing stimulation by SAC, but not when added to unstimulated B cells. Inasmuch as SAC is known to stimulate human B cells by interaction of its cell wall protein A with B cell surface Ig, we propose that the two signals required for B cell stimulation by SAC are identical to those required for responses to specific antigens, and that the present system allows an assay for T cell-derived differentiation factors acting on B cells that have undergone direct antigenic stimulation or its equivalent.

Bibliography

Falkoff, R. J., Zhu, L. P., & Fauci, A. S. (1982). Separate signals for human B cell proliferation and differentiation in response to Staphylococcus aureus: evidence for a two-signal model of B cell activation. The Journal of Immunology, 129(1), 97â102.

Authors 3

R J Falkoff (first)
L P Zhu (additional)
A S Fauci (additional)

References 0 Referenced 122

None

Dates

Type	When
Created	2 years, 8 months ago (Dec. 30, 2022, 8:19 p.m.)
Deposited	5 months ago (March 31, 2025, 5:25 p.m.)
Indexed	5 months ago (April 1, 2025, 12:13 a.m.)
Issued	43 years, 2 months ago (July 1, 1982)
Published	43 years, 2 months ago (July 1, 1982)
Published Online	43 years, 2 months ago (July 1, 1982)
Published Print	43 years, 2 months ago (July 1, 1982)

Funders 0

None

BibTeX

@article{Falkoff_1982, title={Separate signals for human B cell proliferation and differentiation in response to Staphylococcus aureus: evidence for a two-signal model of B cell activation.}, volume={129}, ISSN={1550-6606}, url={http://dx.doi.org/10.4049/jimmunol.129.1.97}, DOI={10.4049/jimmunol.129.1.97}, number={1}, journal={The Journal of Immunology}, publisher={Oxford University Press (OUP)}, author={Falkoff, R J and Zhu, L P and Fauci, A S}, year={1982}, month=jul, pages={97–102} }

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