Journal of Experimental Medicine, Vol 148, 1628-1643, Copyright © 1978 by Rockefeller University Press

ARTICLES

Activation of mouse lymphocytes by anti-immunoglobulin. II. A thymus- independent response by a mature subset of B lymphocytes

DG Sieckmann, I Scher, R Asofsky, DE Mosier and WE Paul

Mouse spleen cells can be stimulated to proliferate in vitro by purified anti-mu or anti-gamma,kappa antibodies. These responses can be obtained in cell populations bearing membrane immunoglobulin (Ig), purified by the fluorescence activated cell sorter (FACS), but they are not observed in FACS-purified Ig- cell populations. Furthermore, treatment of spleen cell populations with anti-Thy 1.2 and complement does not impair the response, nor does addition of nylon wool-purified T lymphocytes enhance it. These results indicate that B lymphocytes respond to anti-Ig and that their response does not require T cells. On the other hand, cells from athymic nude (nu/nu) mice respond slightly less well to anti-mu than do cells from heterozygous littermate (nu/+) controls; nu/nu cells are almost unresponsive to anti-gamm,kappa and addition of nylon wool-purified T cells from nu/+ controls does not restore the response. This suggests that T lymphocytes or the thymus may control the appearance of cells responsive to anti-gamma,kappa. Responsiveness of normal mice to anti-mu does not appear until 4 wk of age and does not reach maximum levels until 8 wk of age. Acquisition of full responsiveness to anti-gamma,kappa is even more delayed. This, together with the failure of mice with the CBA/N B-cell defect to respond to anti-Ig, suggests that cells stimulated to proliferate by anti-Ig are a mature subset of B cells. Depletion of adherent cells by Sephadex G-10 treatment or by treatment with carbonyl iron and exposure to a magnetic field does not diminish anti-mu or anti-gamma,kappa responses, suggesting that the responsiveness does not require the presence of macrophages. Thus, activation of B-cell proliferation by anti-Ig appears to be a T-cell independent, macrophage-independent process in which membrane Ig plays a direct role in signal generation.
CiteULike    Complore    Connotea    Del.icio.us    Digg    Facebook    Reddit    Technorati    Twitter    What's this?

This article has been cited by other articles:

• Cabatingan, M. S., Schmidt, M. R., Sen, R., Woodland, R. T. (2002). Naive B Lymphocytes Undergo Homeostatic Proliferation in Response to B Cell Deficit. J. Immunol. 169: 6795-6805 [Abstract] [Full Text]  
• Su, T. T., Rawlings, D. J. (2002). Transitional B Lymphocyte Subsets Operate as Distinct Checkpoints in Murine Splenic B Cell Development. J. Immunol. 168: 2101-2110 [Abstract] [Full Text]  
• Cancro, M. P., Sah, A. P., Levy, S. L., Allman, D. M., Schmidt, M. R., Woodland, R. T. (2001). xid mice reveal the interplay of homeostasis and Bruton's tyrosine kinase-mediated selection at multiple stages of B cell development. Int Immunol 13: 1501-1514 [Abstract] [Full Text]  
• Arnold, L. W., McCray, S. K., Tatu, C., Clarke, S. H. (2000). Identification of a Precursor to Phosphatidyl Choline-Specific B-1 Cells Suggesting That B-1 Cells Differentiate from Splenic Conventional B Cells In Vivo: Cyclosporin A Blocks Differentiation to B-1. J. Immunol. 164: 2924-2930 [Abstract] [Full Text]  
• Clarke, S. H., Arnold, L. W. (1998). B-1 Cell Development: Evidence for an Uncommitted Immunoglobulin (Ig)M+ B Cell Precursor in B-1 Cell Differentiation. JEM 187: 1325-1334 [Abstract] [Full Text]  
• Solvason, N., Wu, W. W., Kabra, N., Lund-Johansen, F., Roncarolo, M. G., Behrens, T. W., Grillot, D. A.M., Nunez, G., Lees, E., Howard, M. (1998). Transgene Expression of bcl-xL Permits Anti-immunoglobulin (Ig)-induced Proliferation in xid B Cells. JEM 187: 1081-1091 [Abstract] [Full Text]  

Home | Help | Feedback | Subscriptions | Archive | Search

TABLE OF CONTENTS