Immunotherapy of a murine tumor with interleukin 2. Increased sensitivity after MHC class I gene transfection

doi:10.1084/jem.166.6.1716

This Article

	Full Text (PDF, 1124K)
	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 Weber, J. S.
	Articles by Rosenberg, S. A.
	Search for Related Content

PubMed

	PubMed Citation
	Articles by Weber, J. S.
	Articles by Rosenberg, S. A.


Social Bookmarking

	What's this?

ARTICLES

Immunotherapy of a murine tumor with interleukin 2. Increased sensitivity after MHC class I gene transfection

JS Weber, G Jay, K Tanaka and SA Rosenberg
Surgery Branch, National Cancer Institute, Bethesda, Maryland 20892.

We have shown that two weakly immunogenic MCA sarcomas developed in our laboratory that are sensitive to high-dose IL-2 immunotherapy express class I MHC in vivo and in vitro. Two nonimmunogenic MCA sarcomas are relatively insensitive to IL-2 therapy and express minimal or no class I MHC molecules in vivo and in vitro. To study the role of MHC in the therapy of tumors with IL-2, a class I-deficient murine melanoma, B16BL6, was transfected with the Kb class I gene. Expression of class I MHC rendered B16BL6 advanced pulmonary macrometastases sensitive to IL- 2 immunotherapy. 3-d micrometastases of CL8-2, a class I transfected clone of B16BL6, were significantly more sensitive to IL-2 therapy than a control nontransfected line. Expression of Iak, a class II MHC molecule, had no effect on IL-2 therapy of transfectant pulmonary micrometastases in F1 mice. By using lymphocyte subset depletion with mAbs directed against Lyt-2, therapy of class I transfectant macrometastases with high-dose IL-2 was shown to involve an Lyt-2 cell. In contrast, regression of micrometastases treated with low-dose IL-2 involved Lyt-2+ cells, but regression mediated by high doses of IL-2 did not. We hypothesize that both LAK and Lyt-2+ T cells effect IL-2- mediated elimination of micrometastases, but only Lyt-2+ T cells are involved in macrometastatic regression. Low doses of IL-2 stimulate Lyt- 2+ cells to eliminate class I-expressing micrometastases, but high doses of IL-2 can recruit LAK cells to mediate regression of micrometastases independent of class I expression. Only high-dose IL-2, mediating its effect predominantly via Lyt-2+ cells, is capable of impacting on MHC class I-expressing macrometastases. Macrometastases devoid of class I MHC antigens appear to be resistant to IL-2 therapy.
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:

Gollob, J. A., Sciambi, C. J., Peterson, B. L., Richmond, T., Thoreson, M., Moran, K., Dressman, H. K., Jelinek, J., Issa, J.-P. J. (2006). Phase I Trial of Sequential Low-Dose 5-Aza-2'-Deoxycytidine Plus High-Dose Intravenous Bolus Interleukin-2 in Patients with Melanoma or Renal Cell Carcinoma. Clin. Cancer Res. 12: 4619-4627 [Abstract] [Full Text]
Segal, J. G., Lee, N. C., Tsung, Y. L., Norton, J. A., Tsung, K. (2002). The Role of IFN-{gamma} in Rejection of Established Tumors by IL-12 : Source of Production and Target. Cancer Res. 62: 4696-4703 [Abstract] [Full Text]
Kirk, C. J., Hartigan-O'Connor, D., Mule, J. J. (2001). The Dynamics of the T-Cell Antitumor Response: Chemokine-secreting Dendritic Cells Can Prime Tumor-reactive T Cells Extranodally. Cancer Res. 61: 8794-8802 [Abstract] [Full Text]
Winter, H., Hu, H.-M., McClain, K., Urba, W. J., Fox, B. A. (2001). Immunotherapy of Melanoma: A Dichotomy in the Requirement for IFN-{{gamma}} in Vaccine-Induced Antitumor Immunity Versus Adoptive Immunotherapy. J. Immunol. 166: 7370-7380 [Abstract] [Full Text]
Shimizu, K., Thomas, E. K., Giedlin, M., Mulé, J. J. (2001). Enhancement of Tumor Lysate- and Peptide-pulsed Dendritic Cell-based Vaccines by the Addition of Foreign Helper Protein. Cancer Res. 61: 2618-2624 [Abstract] [Full Text]
Winter, H., Hu, H.-M., Urba, W. J., Fox, B. A. (1999). Tumor Regression After Adoptive Transfer of Effector T Cells Is Independent of Perforin or Fas Ligand (APO-1L/CD95L). J. Immunol. 163: 4462-4472 [Abstract] [Full Text]
Strome, S. E., Krauss, J. C., Cameron, M. J., Forslund, K., Shu, S., Chang, A. E. (1993). Immunobiologic Effects of Cytokine Gene Transfer of the B16-BL6 Melanoma. Arch Otolaryngol Head Neck Surg 119: 1289-1295 [Abstract]
Sigal, R. K., Lieberman, M. D., Reynolds, J. V., Williams, N., Ziegler, M. M., Daly, J. M. (1990). Tumor Immunization: Improved Results After Vaccine Modified With Recombinant Interferon Gamma. Arch Surg 125: 308-312 [Abstract]