Literature DB >> 11724951

Role of SEREX-defined immunogenic wild-type cellular molecules in the development of tumor-specific immunity.

H Nishikawa1, K Tanida, H Ikeda, M Sakakura, Y Miyahara, T Aota, K Mukai, M Watanabe, K Kuribayashi, L J Old, H Shiku.   

Abstract

Recognition of altered self-antigens in tumor cells by lymphocytes forms the basis for antitumor immune responses. The effector cells in most experimental tumor systems are CD8(+) T cells that recognize MHC class I binding peptides derived from molecules with altered expression in tumor cells. Although the need for CD4(+) helper T cells in regulating CD8(+) T cells has been documented, their target epitopes and functional impact in antitumor responses remain unclear. We examined whether broadly expressed wild-type molecules in murine tumor cells eliciting humoral immunity contributed to the generation of CD8(+) T cells and protective antitumor immune responses to unrelated tumor-specific antigens [mutated ERK2 (mERK2) and c-erbB2/HER/neu (HER2)]. The immunogenic wild-type molecules, presumably dependent on recognition by CD4(+) helper T cells, were defined by serological analysis of recombinant cDNA expression libraries (SEREX) using tumor-derived lambda phage libraries screened with IgG antibodies of hosts bearing transplanted 3-methylchoranthrene-induced tumors. Coimmunization of mice with plasmids encoding SEREX-defined murine wild-type molecules and mERK2 or HER2 led to a profound increase in CD8(+) T cells specific for mERK2 or HER2 peptides. This heightened response depended on CD4(+) T cells and copresentation of SEREX-defined molecules and CD8(+) T cell epitopes. In tumor protection assays, immunization with SEREX-defined wild-type molecules and mERK2 resulted in an inhibition of pulmonary metastasis, which was not achieved by immunization with mERK2 alone.

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Year:  2001        PMID: 11724951      PMCID: PMC64723          DOI: 10.1073/pnas.251547298

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  42 in total

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4.  Efficient selection for high-expression transfectants with a novel eukaryotic vector.

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5.  Mutated mitogen-activated protein kinase: a tumor rejection antigen of mouse sarcoma.

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9.  Influence of interleukin 12 on p53 peptide vaccination against established Meth A sarcoma.

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  15 in total

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