Cell therapy method for the treatment of tumors

摘要

T cell responses are often diminished in humans with a compromised immune system. We have developed a method to isolate, stimulate and expand naïve cytotoxic T lymphocyte precursors (CTLp) to antigen-specific effectors, capable of lysing tumor cells in vivo. This ex vivo protocol produces fully functional effectors. Artificial antigen presenting cells (AAPCs; Drosophila melanogaster) transfected with human HLA class I and defined accessory molecules, are used to stimulate CD8+ T cells from both normal donors and cancer patients. The class I molecules expressed to a high density on the surface of the Drosophila cells are empty, allowing for efficient loading of multiple peptides that results in the generation of polyclonal responses recognizing tumor cells endogenously expressing the specific peptides. The responses generated are robust, antigen-specific and reproducible if the peptide epitope is a defined immunogen. This artificial antigen expression system can be adapted to treat most cancers in a significant majority of the population.

主权项

1. A method for producing activated CD8+ T cells specific to one or more melanoma antigens for administration to a subject, comprising:
a. harvesting CD8+ T cells and CD8-depeleted mononuclear cells from the subject; b. culturing said CD8+ T cells with a non-naturally occurring antigen-presenting cell line (nnAPC) presenting one or more melanoma antigenic peptides for a period of time sufficient for activation of CD8+ T cells that are specific for the melanoma antigenic peptides, wherein the melanoma antigenic peptides have the amino acid sequences of peptide fragments of one or more melanoma-associated antigens; wherein at least one of the melanoma-associated antigens is selected from the group consisting of tvrosinase, gp100, and MART-1, and wherein said melanoma antigenic peptides are each about six to twelve amino acids in length; c. adding said CD8+ T cells to media that contains at least one cytokine selected from the group consisting of IL-2, IL-7 or conditioned growth medium (CGM), wherein said cytokines can be used individually or in combination to expand the CD8+ T cells; d. irradiating said CD8-depleted mononuclear cells with a sufficient dose of γ-radiation to prevent proliferation of said CD8-depleted mononuclear cells; e. isolating adherent CD8-depleted mononuclear cells from the irradiated cells; f. loading the CD8-depleted mononuclear cells with about 1 to 50 μg/ml of the melanoma antigenic peptides; g. restimulating said CD8+ T cells by mixing said CD8+ T cells with the peptide-loaded CD8-depleted mononuclear cells at a ratio of about ten CD8+ T cells to one CD8-depleted mononuclear cells; h. expanding the CD8+ T cells; and i. inoculating the subject with collecting the activated CD8+ T cells specific to melanoma antigenic peptides for administration to the subject.