Literature DB >> 14738463

IL-12 enhances the generation of tumour antigen-specific Th1 CD4 T cells during ex vivo expansion.

K L Knutson1, M L Disis.   

Abstract

CD4+ T cells are essential for the immune response against cancer. Vaccination against cancer will likely only be effective at preventing growth of micrometastatic disease while adoptive T cell therapy will be better suited for eradication of bulky pre-existing disease (Knutson et al. Expert Opin Biol Ther 2002; 2:55-66). Problems with the use of adoptive T cell therapy include lack of CD4+ T cell help, low frequency of antigen-specific T cells, and lack of effective ex vivo expansion techniques. In this study, we focused on improving ex vivo expansion of CD4+ T helper cells. The effects of IL-12, along with IL-2, on the ex vivo generation of HER-2/neu antigen-specific T cells were examined. Patients were immunized with a peptide-based vaccine that contained a helper epitope, p776-790, derived from the intracellular domain of HER-2/neu. While T cell immunity to p776-790, assessed by proliferation assays, could be readily measured in short-term cultures, cell line generation by multiple in vitro stimulation with peptide and IL-2 as the only added cytokine resulted in loss of antigen-specific proliferation. The inclusion of IL-12, along with IL-2, restored antigen-specific proliferation in a dose-dependent fashion. The resulting p776-790-specific T cells responded readily to antigen by proliferating and producing type I cytokines (IFN-gamma and TNF-alpha). The increased proliferative response of the cultures was due in part to an increase in the number of HER-2/neu-specific T cells. These results suggest that IL-12 is an important cytokine for ex vivo recovery and maintenance of antigen-specific CD4+ T lymphocytes that would otherwise be lost by using IL-2 alone in combination with antigen. Furthermore, these results have important implications for ex vivo expansion of CD4+ T cell for use in anti-tumour adoptive immunotherapy.

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Year:  2004        PMID: 14738463      PMCID: PMC1808930          DOI: 10.1111/j.1365-2249.2004.02360.x

Source DB:  PubMed          Journal:  Clin Exp Immunol        ISSN: 0009-9104            Impact factor:   4.330


  30 in total

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Journal:  J Immunol       Date:  2001-03-15       Impact factor: 5.422

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Authors:  Mary L Disis; Theodore A Gooley; Kristine Rinn; Donna Davis; Michael Piepkorn; Martin A Cheever; Keith L Knutson; Kathy Schiffman
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Authors:  H M Hu; H Winter; W J Urba; B A Fox
Journal:  J Immunol       Date:  2000-10-15       Impact factor: 5.422

Review 7.  Expansion of HER2/neu-specific T cells ex vivo following immunization with a HER2/neu peptide-based vaccine.

Authors:  K L Knutson; M L Disis
Journal:  Clin Breast Cancer       Date:  2001-04       Impact factor: 3.225

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9.  Repeated administrations of interleukin (IL)-12 are associated with persistently elevated plasma levels of IL-10 and declining IFN-gamma, tumor necrosis factor-alpha, IL-6, and IL-8 responses.

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10.  Clonal diversity of the T-cell population responding to a dominant HLA-A2 epitope of HER-2/neu after active immunization in an ovarian cancer patient.

Authors:  Keith L Knutson; Mary L Disis
Journal:  Hum Immunol       Date:  2002-07       Impact factor: 2.850

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5.  HER-2/neu vaccine-primed autologous T-cell infusions for the treatment of advanced stage HER-2/neu expressing cancers.

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6.  Immunomodulation of breast cancer via tumor antigen specific Th1.

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Journal:  Cancer Res Treat       Date:  2009-09-28       Impact factor: 4.679

7.  The Antitumor Efficacy of IL2/IL21-Cultured Polyfunctional Neu-Specific T Cells Is TNFα/IL17 Dependent.

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8.  Surrogate in vitro activation of innate immunity synergizes with interleukin-7 to unleash rapid antigen-driven outgrowth of CD4+ and CD8+ human peripheral blood T-cells naturally recognizing MUC1, HER2/neu and other tumor-associated antigens.

Authors:  Latha B Pathangey; Dustin B McCurry; Sandra J Gendler; Ana L Dominguez; Jessica E Gorman; Girish Pathangey; Laurie A Mihalik; Yushe Dang; Mary L Disis; Peter A Cohen
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9.  Combination of dual mTORC1/2 inhibition and immune-checkpoint blockade potentiates anti-tumour immunity.

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