A disease-related rheumatoid factor autoantibody is not tolerized in a normal mouse: implications for the origins of autoantibodies in autoimmune disease

doi:10.1084/jem.184.4.1269

This Article

	Full Text (PDF, 970K)
	Alert me when this article is cited
	Citation Map

Services

	Email this article
	Similar articles in this journal
	Similar articles in PubMed
	Alert me to new content in the JEM
	Download to citation manager

Citing Articles

	Citing Articles via HighWire
	Citing Articles via CrossRef
	Citing Articles via Google Scholar

Google Scholar

	Articles by Hannum, L. G.
	Articles by Shlomchik, M. J.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Hannum, L. G.
	Articles by Shlomchik, M. J.


Social Bookmarking

	What's this?

ARTICLES

A disease-related rheumatoid factor autoantibody is not tolerized in a normal mouse: implications for the origins of autoantibodies in autoimmune disease

LG Hannum, D Ni, AM Haberman, MG Weigert and MJ Shlomchik
Section of Immunobiology, Yale University School of Medicine, New Haven, Connecticut 06520, USA.

We have analyzed B cell tolerance in a rheumatoid factor (RF) transgenic mouse model. The model is based on AM14, a hybridoma, originally isolated from an autoimmune MRL/lpr mouse that has an affinity and specificity typical of disease-related RFs from this strain. AM14 binds to immunoglobulin (Ig)G2a of the "a" allotype (IgG2aa) and not to IgG2ab. Thus, by crossing the transgenes onto an IgHa (BALB/c) background or to a congenic IgHb (CB.17) background, we could study the RF-expressing B cells when they were self-specific (IgHa) or when they were not self-specific (IgHb). These features make the AM14 model unique in focusing on a true autoantibody specificity while at the same time allowing comparison of autoreactive and nonautoreactive transgenic B cells, as was possible in model autoantibody systems such as anti-hen egg lysozyme. Studies showed that AM14 RF B cells can make primary immune responses and do not downregulate sIgM, indicating that the presence of self-antigen does not induce anergy of these cells. In fact, IgHa AM14 transgenic mice have higher serum levels of transgene-encoded RF than their IgHb counterparts, suggesting that self-antigen-specific activation occurs even in the normal mouse background. Since AM14 B cells made primary responses, we had the opportunity to test for potential blocks to self- reactive cells entering the memory compartment. We did not find evidence of this, as AM14 B cells made secondary immune responses as well. These data demonstrate that a precursor of a disease-specific autoantibody can be present in the preimmune repertoire and functional even to the point of memory cell development of normal mice. Therefore, immunoregulatory mechanisms that normally prevent autoantibody production must exert their effects later in B cell development or through T cell tolerance. Conversely, the data suggest that it is not necessary to break central tolerance, even in an autoimmune mouse, to generate pathologic, disease-associated autoantibodies.
Add to CiteULike CiteULike Add to Complore Complore Add to Connotea Connotea Add to Del.icio.us Del.icio.us Add to Digg Digg Add to Reddit Reddit Add to Technorati Technorati What's this?

This article has been cited by other articles:

Tomayko, M. M., Anderson, S. M., Brayton, C. E., Sadanand, S., Steinel, N. C., Behrens, T. W., Shlomchik, M. J. (2008). Systematic Comparison of Gene Expression between Murine Memory and Naive B Cells Demonstrates That Memory B Cells Have Unique Signaling Capabilities. J. Immunol. 181: 27-38 [Abstract] [Full Text]
Kiefer, K., Nakajima, P. B., Oshinsky, J., Seeholzer, S. H., Radic, M., Bosma, G. C., Bosma, M. J. (2008). Antigen Receptor Editing in Anti-DNA Transitional B Cells Deficient for Surface IgM. J. Immunol. 180: 6094-6106 [Abstract] [Full Text]
Ahuja, A., Anderson, S. M., Khalil, A., Shlomchik, M. J. (2008). Maintenance of the plasma cell pool is independent of memory B cells. Proc. Natl. Acad. Sci. USA 105: 4802-4807 [Abstract] [Full Text]
Busconi, L., Bauer, J. W., Tumang, J. R., Laws, A., Perkins-Mesires, K., Tabor, A. S., Lau, C., Corley, R. B., Rothstein, T. L., Lund, F. E., Behrens, T. W., Marshak-Rothstein, A. (2007). Functional Outcome of B Cell Activation by Chromatin Immune Complex Engagement of the B Cell Receptor and TLR9. J. Immunol. 179: 7397-7405 [Abstract] [Full Text]
Kilmon, M. A., Wagner, N. J., Garland, A. L., Lin, L., Aviszus, K., Wysocki, L. J., Vilen, B. J. (2007). Macrophages prevent the differentiation of autoreactive B cells by secreting CD40 ligand and interleukin-6. Blood 110: 1595-1602 [Abstract] [Full Text]
Yan, J., Harvey, B. P., Gee, R. J., Shlomchik, M. J., Mamula, M. J. (2006). B Cells Drive Early T Cell Autoimmunity In Vivo prior to Dendritic Cell-Mediated Autoantigen Presentation. J. Immunol. 177: 4481-4487 [Abstract] [Full Text]
Mandik-Nayak, L., Racz, J., Sleckman, B. P., Allen, P. M. (2006). Autoreactive marginal zone B cells are spontaneously activated but lymph node B cells require T cell help. JEM 203: 1985-1998 [Abstract] [Full Text]
Beaudette-Zlatanova, B. C., Ling, T., Shlomchik, M. J., Marshak-Rothstein, A., Rifkin, I. R. (2006). B Cells and Dendritic Cells from V{kappa}8 Light Chain Transgenic Mice Activate MRL-lpr/gld CD4+ T Cells. J. Immunol. 177: 45-52 [Abstract] [Full Text]
Nijnik, A., Ferry, H., Lewis, G., Rapsomaniki, E., Leung, J. C. H., Daser, A., Lambe, T., Goodnow, C. C., Cornall, R. J. (2006). Spontaneous B cell hyperactivity in autoimmune-prone MRL mice. Int Immunol 18: 1127-1137 [Abstract] [Full Text]
William, J., Euler, C., Primarolo, N., Shlomchik, M. J. (2006). B Cell Tolerance Checkpoints That Restrict Pathways of Antigen-Driven Differentiation. J. Immunol. 176: 2142-2151 [Abstract] [Full Text]
William, J., Euler, C., Leadbetter, E., Marshak-Rothstein, A., Shlomchik, M. J. (2005). Visualizing the Onset and Evolution of an Autoantibody Response in Systemic Autoimmunity. J. Immunol. 174: 6872-6878 [Abstract] [Full Text]
William, J., Euler, C., Shlomchik, M. J. (2005). Short-Lived Plasmablasts Dominate the Early Spontaneous Rheumatoid Factor Response: Differentiation Pathways, Hypermutating Cell Types, and Affinity Maturation Outside the Germinal Center. J. Immunol. 174: 6879-6887 [Abstract] [Full Text]
Guay, H. M., Panarey, L., Reed, A. J., Caton, A. J. (2004). Specificity-Based Negative Selection of Autoreactive B Cells during Memory Formation. J. Immunol. 173: 5485-5494 [Abstract] [Full Text]
Marshak-Rothstein, A., Busconi, L., Lau, C. M., Tabor, A. S., Leadbetter, E. A., Akira, S., Krieg, A. M., Lipford, G. B., Viglianti, G. A., Rifkin, I. R. (2004). Comparison of CpG s-ODNs, chromatin immune complexes, and dsDNA fragment immune complexes in the TLR9-dependent activation of rheumatoid factor B cells. Innate Immunity 10: 247-251 [Abstract]
Widhopf, G. F. II, Brinson, D. C., Kipps, T. J., Tighe, H. (2004). Transgenic Expression of a Human Polyreactive Ig Expressed in Chronic Lymphocytic Leukemia Generates Memory-Type B Cells That Respond to Nonspecific Immune Activation. J. Immunol. 172: 2092-2099 [Abstract] [Full Text]
Meffre, E., Schaefer, A., Wardemann, H., Wilson, P., Davis, E., Nussenzweig, M. C. (2004). Surrogate Light Chain Expressing Human Peripheral B Cells Produce Self-reactive Antibodies. JEM 199: 145-150 [Abstract] [Full Text]
Aplin, B. D., Keech, C. L., de Kauwe, A. L., Gordon, T. P., Cavill, D., McCluskey, J. (2003). Tolerance through Indifference: Autoreactive B Cells to the Nuclear Antigen La Show No Evidence of Tolerance in a Transgenic Model. J. Immunol. 171: 5890-5900 [Abstract] [Full Text]
Ferry, H., Jones, M., Vaux, D. J., Roberts, I. S.D., Cornall, R. J. (2003). The Cellular Location of Self-antigen Determines the Positive and Negative Selection of Autoreactive B Cells. JEM 198: 1415-1425 [Abstract] [Full Text]
Hayakawa, K., Asano, M., Shinton, S. A., Gui, M., Wen, L.-J., Dashoff, J., Hardy, R. R. (2003). Positive Selection of Anti-Thy-1 Autoreactive B-1 Cells and Natural Serum Autoantibody Production Independent from Bone Marrow B Cell Development. JEM 197: 87-99 [Abstract] [Full Text]
William, J., Euler, C., Christensen, S., Shlomchik, M. J. (2002). Evolution of Autoantibody Responses via Somatic Hypermutation Outside of Germinal Centers. Science 297: 2066-2070 [Abstract] [Full Text]
Yan, J., Mamula, M. J. (2002). B and T cell tolerance and autoimmunity in autoantibody transgenic mice. Int Immunol 14: 963-971 [Abstract] [Full Text]
Santulli-Marotto, S., Qian, Y., Ferguson, S., Clarke, S. H. (2001). Anti-Sm B Cell Differentiation in Ig Transgenic MRL/Mp-lpr/lpr Mice: Altered Differentiation and an Accelerated Response. J. Immunol. 166: 5292-5299 [Abstract] [Full Text]
Rojas, M., Hulbert, C., Thomas, J. W. (2001). Anergy and not Clonal Ignorance Determines the Fate of B Cells that Recognize a Physiological Autoantigen. J. Immunol. 166: 3194-3200 [Abstract] [Full Text]
Koh, J. S., Wang, Z., Levine, J. S. (2000). Cytokine Dysregulation Induced by Apoptotic Cells Is a Shared Characteristic of Murine Lupus. J. Immunol. 165: 4190-4201 [Abstract] [Full Text]
Rifkin, I. R., Leadbetter, E. A., Beaudette, B. C., Kiani, C., Monestier, M., Shlomchik, M. J., Marshak-Rothstein, A. (2000). Immune Complexes Present in the Sera of Autoimmune Mice Activate Rheumatoid Factor B Cells. J. Immunol. 165: 1626-1633 [Abstract] [Full Text]
Wang, H., Shlomchik, M. J. (1999). Autoantigen-specific B Cell Activation in Fas-deficient Rheumatoid Factor Immunoglobulin Transgenic Mice. JEM 190: 639-650 [Abstract] [Full Text]
Hayakawa, K., Asano, M., Shinton, S. A., Gui, M., Allman, D., Stewart, C. L., Silver, J., Hardy, R. R. (1999). Positive Selection of Natural Autoreactive B Cells. Science 285: 113-116 [Abstract] [Full Text]
Jemmerson, R., Minnerath, J. M., Hedrick, S. M., Oehen, S. (1998). B Cell Tolerance to a Minor, But Not to a Major, Antigenic Surface of the Self Antigen, Cytochrome c. J. Immunol. 161: 2841-2847 [Abstract] [Full Text]
Lecerf, J.-M., Chen, Y., Richalet-Secordel, P., Wang, X., Stollar, B. D. (1998). Autoreactivity of Human VH Domains from cDNA Libraries: Analysis with a Bacterial Expression System. J. Immunol. 161: 1274-1283 [Abstract] [Full Text]
Wang, H., Shlomchik, M. J. (1998). Maternal Ig Mediates Neonatal Tolerance in Rheumatoid Factor Transgenic Mice but Tolerance Breaks Down in Adult Mice. J. Immunol. 160: 2263-2271 [Abstract] [Full Text]
Dal Porto, J. M., Haberman, A. M., Kelsoe, G., Shlomchik, M. J. (2002). Very Low Affinity B Cells Form Germinal Centers, Become Memory B Cells, and Participate in Secondary Immune Responses When Higher Affinity Competition Is Reduced. JEM 195: 1215-1221 [Abstract] [Full Text]