Immunologically mediated regression of a murine lymphoma after treatment with anti-L3T4 antibody. A consequence of removing L3T4+ suppressor T cells from a host generating predominantly Lyt-2+ T cell- mediated immunity

doi:10.1084/jem.168.6.2193

This Article

	Full Text (PDF)
	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 Awwad, M.
	Articles by North, R. J.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Awwad, M.
	Articles by North, R. J.


Social Bookmarking

	What's this?

ARTICLES

Immunologically mediated regression of a murine lymphoma after treatment with anti-L3T4 antibody. A consequence of removing L3T4+ suppressor T cells from a host generating predominantly Lyt-2+ T cell- mediated immunity

M Awwad and RJ North
Trudeau Institute, Saranac Lake, New York 12983.

This study shows that intravenous injection of 1 mg of anti-L3T4 mAb (GK1.5) into thymectomized mice bearing the syngeneic L5178Y lymphoma results, after a delay of 2-3 d, in complete regression of this tumor and in long-term host survival. A flow cytofluorometric examination of the spleen cells of mAb-treated mice revealed that antibody treatment resulted in the elimination of greater than 98% of L3T4+ T cells, but had no effect on the Lyt-2+ T cells subset. Tumor regression was immunologically mediated, because L5178Y lymphoma cells were shown to be L3T4-, and regression of the tumor failed to occur in mice that had been lethally irradiated before anti-L3T4 mAb was given. Tumor regression was mediated by tumor-sensitized Lyt2+ T cells, as evidenced by the finding that treatment of tumor-bearing mice with anti-Lyt-2 mAb alone, or in combination with anti-L3T4 mAb, resulted in enhancement of tumor growth and a significant decrease in host survival time. Moreover, the spleens of mice whose tumors were undergoing regression in response to anti-L3T4 mAb treatment contained Lyt-2+ T cells capable, on passive transfer, of causing regression of a tumor in recipient mice. These results can be interpreted as showing that removal of tumor-induced L3T4+ suppressor T cells results in the release of Lyt-2+ effector T cells from suppression, and consequently in the generation of enough Lyt-2+ T cell-mediated immunity to cause tumor regression. This can only be achieved, however, if immunity to the tumor is mediated exclusively by Lyt-2+ T cells, as is the case for the L5178Y lymphoma. In the case of the P815 mastocytoma, treatment with anti-L3T4 mAb was without a therapeutic effect, and this was in keeping with the finding that immunity to this tumor is mediated by L3T4+, as well by Lyt-2+ T cells.
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:

Gough, M. J., Ruby, C. E., Redmond, W. L., Dhungel, B., Brown, A., Weinberg, A. D. (2008). OX40 Agonist Therapy Enhances CD8 Infiltration and Decreases Immune Suppression in the Tumor. Cancer Res. 68: 5206-5215 [Abstract] [Full Text]
Webster, W. S., Thompson, R. H., Harris, K. J., Frigola, X., Kuntz, S., Inman, B. A., Dong, H. (2007). Targeting Molecular and Cellular Inhibitory Mechanisms for Improvement of Antitumor Memory Responses Reactivated by Tumor Cell Vaccine. J. Immunol. 179: 2860-2869 [Abstract] [Full Text]
Nitcheu-Tefit, J., Dai, M.-S., Critchley-Thorne, R. J., Ramirez-Jimenez, F., Xu, M., Conchon, S., Ferry, N., Stauss, H. J., Vassaux, G. (2007). Listeriolysin O Expressed in a Bacterial Vaccine Suppresses CD4+CD25high Regulatory T Cell Function In Vivo. J. Immunol. 179: 1532-1541 [Abstract] [Full Text]
Viehl, C. T., Moore, T. T., Liyanage, U. K., Frey, D. M., Ehlers, J. P., Eberlein, T. J., Goedegebuure, P. S., Linehan, D. C. (2006). Depletion of CD4+CD25+ Regulatory T Cells Promotes a Tumor-Specific Immune Response in Pancreas Cancer-Bearing Mice. Ann. Surg. Oncol. 13: 1252-1258 [Abstract] [Full Text]
Fandrich, F. (2006). Induction of tolerance in clinical organ transplantation. Nephrol Dial Transplant 21: 1170-1173 [Full Text]
Dranoff, G. (2005). The Therapeutic Implications of Intratumoral Regulatory T Cells. Clin. Cancer Res. 11: 8226-8229 [Full Text]
Yu, P., Lee, Y., Liu, W., Krausz, T., Chong, A., Schreiber, H., Fu, Y.-X. (2005). Intratumor depletion of CD4+ cells unmasks tumor immunogenicity leading to the rejection of late-stage tumors. J. Exp. Med. 201: 779-791 [Abstract] [Full Text]
Bluestone, J. A., Tang, Q. (2004). Therapeutic vaccination using CD4+CD25+ antigen-specific regulatory T cells. Proc. Natl. Acad. Sci. USA 101: 14622-14626 [Abstract] [Full Text]
Chen, Y.-L., Chen, S.-H., Wang, J.-Y., Yang, B.-C. (2003). Fas Ligand on Tumor Cells Mediates Inactivation of Neutrophils. J. Immunol. 171: 1183-1191 [Abstract] [Full Text]
Liyanage, U. K., Moore, T. T., Joo, H.-G., Tanaka, Y., Herrmann, V., Doherty, G., Drebin, J. A., Strasberg, S. M., Eberlein, T. J., Goedegebuure, P. S., Linehan, D. C. (2002). Prevalence of Regulatory T Cells Is Increased in Peripheral Blood and Tumor Microenvironment of Patients with Pancreas or Breast Adenocarcinoma. J. Immunol. 169: 2756-2761 [Abstract] [Full Text]
Shimizu, J., Yamazaki, S., Sakaguchi, S. (1999). Induction of Tumor Immunity by Removing CD25+CD4+ T Cells: A Common Basis Between Tumor Immunity and Autoimmunity. J. Immunol. 163: 5211-5218 [Abstract] [Full Text]
Onizuka, S., Tawara, I., Shimizu, J., Sakaguchi, S., Fujita, T., Nakayama, E. (1999). Tumor Rejection by in Vivo Administration of Anti-CD25 (Interleukin-2 Receptor {{alpha}}) Monoclonal Antibody. Cancer Res. 59: 3128-3133 [Abstract] [Full Text]
Matsuo, M., Wada, H., Honda, S., Tawara, I., Uenaka, A., Kanematsu, T., Nakayama, E. (1999). Expression of Multiple Unique Rejection Antigens on Murine Leukemia BALB/c RL[IMAGE]1 and the Role of Dominant Akt Antigen for Tumor Escape. J. Immunol. 162: 6420-6425 [Abstract] [Full Text]
Marzo, A. L., Lake, R. A., Robinson, B. W. S., Scott, B. (1999). T-Cell Receptor Transgenic Analysis of Tumor-specific CD8 and CD4 Responses in the Eradication of Solid Tumors. Cancer Res. 59: 1071-1079 [Abstract] [Full Text]
Salgame, P, Abrams, J., Clayberger, C, Goldstein, H, Convit, J, Modlin, R., Bloom, B. (1991). Differing lymphokine profiles of functional subsets of human CD4 and CD8 T cell clones. Science 254: 279-282 [Abstract]