Differences in the repertoire of the Lewis rat T cell response to self and non-self myelin basic proteins

doi:10.1084/jem.167.2.502

This Article

	Full Text (PDF, 656K)
	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 Happ, M. P.
	Articles by Heber-Katz, E.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Happ, M. P.
	Articles by Heber-Katz, E.


Social Bookmarking

	What's this?

ARTICLES

Differences in the repertoire of the Lewis rat T cell response to self and non-self myelin basic proteins

MP Happ and E Heber-Katz
Wistar Institute, Philadelphia, Pennsylvania 19104.

We have examined the fine specificity of a panel of cloned T cell hybridomas generated from Lewis rats immunized with guinea pig (GP) or Lewis rat myelin basic protein (MBP) to determine the autoimmune T cell repertoire that develops in experimental allergic encephalomyelitis (EAE). This analysis has demonstrated that GP MBP, which was approximately 10-fold more potent for EAE induction than the autologous rat MBP, produced a population in which almost one-fourth of the members responded to GP-unique determinants and displayed no crossreactivity on the self antigen. The remaining majority of GP MBP- induced clones were specific for the 68-88 encephalitogenic determinant and could be subdivided into three groups based on their varying responses to the 68-88 peptide and rat and rabbit MBPs. Surprisingly, one of these groups showed equal reactivity to GP and rat MBPs. In contrast, the clonotype composition of the T cell population induced by rat MBP was quite different. One-half of these clones comprised a single group responding to the 68-88 determinant, reacting equally with GP and rat MBP. All of these responded to the same range of antigen concentrations as their GP-induced counterparts. The remaining half of that population contained a collection of clones that was nearly as encephalitogenic as the 68-88 population after propagation as a short- term T cell line. These clones were specific for at least three distinct antigenic determinants, all displaying extensive cross-species reactivity, and required as little or less rat MBP for maximal stimulation as did the 68-88-reactive clones. We therefore conclude that the T cell repertoire for MBP does include clones with reactivity to both 68-88 and non-68-88 determinants of GP and rat MBPs, and that both MBPs appear to be equally capable of stimulating these clones in vitro. However, the differences in the clonotype composition of the populations induced by immunization with these two antigens suggest that rat and GP MBPs are subject to different immunoregulatory constraints in the animal and may account for the difference in the encephalitogenic potential of these two antigens.
Add to CiteULike CiteULike Add to Complore Complore Add to Connotea Connotea Add to Del.icio.us Del.icio.us Add to Digg Digg Facebook Add to Reddit Reddit Add to Technorati Technorati Twitter What's this?

This article has been cited by other articles:

Patel, D. M., Arnold, P. Y., White, G. A., Nardella, J. P., Mannie, M. D. (1999). Class II MHC/Peptide Complexes Are Released from APC and Are Acquired by T Cell Responders During Specific Antigen Recognition. J. Immunol. 163: 5201-5210 [Abstract] [Full Text]
Gregerson, D. S., Torseth, J. W., McPherson, S. W., Roberts, J. P., Shinohara, T., Zack, D. J. (1999). Retinal Expression of a Neo-Self Antigen, {beta}-Galactosidase, Is Not Tolerogenic and Creates a Target for Autoimmune Uveoretinitis. J. Immunol. 163: 1073-1080 [Abstract] [Full Text]
Clark, L., Otvos, L. Jr., Stein, P. L., Zhang, X.-M., Skorupa, A. F., Lesh, G. E., McMorris, F. A., Heber-Katz, E. (1999). Golli-Induced Paralysis: A Study in Anergy and Disease. J. Immunol. 162: 4300-4310 [Abstract] [Full Text]
Weissert, R., Svenningsson, A., Lobell, A., de Graaf, K. L., Andersson, R., Olsson, T. (1998). Molecular and Genetic Requirements for Preferential Recruitment of TCRBV8S2+ T Cells in Lewis Rat Experimental Autoimmune Encephalomyelitis. J. Immunol. 160: 681-690 [Abstract] [Full Text]
Heber-Katz, E. (1989). A New Hierarchy of TCR Specificity: Autoimmune Diseases Are Defined by Particular V{alpha}V{beta} Combinations and Not by Antigen Specificity. Cold Spring Harb Symp Quant Biol 54: 875-878 [Abstract]