MUC1-specific anti-tumor responses: molecular requirements for CD4-mediated responses

doi:10.1093/intimm/dxf053

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International Immunology, Vol. 14, No. 8, pp. 873-882, August 2002
© 2002 Japanese Society for Immunology

MUC1-specific anti-tumor responses: molecular requirements for CD4-mediated responses

Michelle L. VanLith¹, Karl G. Kohlgraf¹, Connie L. Sivinski¹, Richard M. Tempero¹ and Michael A. Hollingsworth¹

¹ Eppley Institute for Research in Cancer and Allied Diseases, and Department of Pathology and Microbiology, University of Nebraska Medical Center, Omaha, NE 68198, USA

Correspondence to: M. A. Hollingsworth; E- mail: mahollin{at}unmc.edu
Transmitting editor: S. L. Swain

MUC1 was first defined as a tumor antigen in the late 1980s,yet little is known about the types of immune responses thatmediate rejection of MUC1⁺ tumors in vivo. MUC1-specific antibodies,T_h cells and cytotoxic T cells can be detected in patients withdifferent adenocarcinomas, yet these tumors usually progress.Thus, there is a need to better understand the in vivo mechanismsof antigen-specific tumor rejection. To characterize the natureof MUC1-specific immune responses in vivo, rejection of a MUC1-expressingmelanoma tumor line (B16.MUC1) was evaluated in mice lackingspecific T cell subsets, cytokines, co-stimulatory moleculesor molecular effectors of cytolytic pathways. Results demonstratedthat rejection of the B16.MUC1 tumor cell line was primarilymediated by CD4⁺ T cells, and required Fas ligand, lymphotoxin- ${alpha}$ ,CD40, CD40 ligand and CD28, but not perforin, ${gamma}$ ${delta}$ T cells, IL-4,IL-10, IL-12 or tumor necrosis factor receptor-1. Depletionof NK cells demonstrated that NK cells might also contributeto MUC1 immunity in the B16.MUC1 tumor model. These resultsdemonstrated that the immune response generated against MUC1does not fit the type 1 or 2 model described for many immuneresponses. Additionally, multiple cytolytic mechanisms are requiredfor B16.MUC1 rejection.

Keywords: cytokines, MUC1, T cells, tumor immunity, tumor vaccine

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