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      Using Human Induced Pluripotent Stem Cells for the Generation of Tumor Antigen-specific T Cells.

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          Abstract

          The generation and expansion of functional T cells in vitro can lead to a broad range of clinical applications. One such use is for the treatment of patients with advanced cancer. Adoptive T cell transfer (ACT) of highly enriched tumor antigen-specific T cells has been shown to cause durable regression of metastatic cancer in some patients. However, during expansion, these cells may become exhausted or senescent, limiting their effector function and persistence in vivo. Induced pluripotent stem cell (iPSC) technology may overcome these obstacles by leading to in vitro generation of large numbers of less differentiated tumor antigen-specific T cells. Human iPSC (hiPSC) have the capacity to differentiate into any type of somatic cell, including lymphocytes, which retain the original T cell receptor (TCR) genomic rearrangement when a T cell is used as a starting cell. Therefore, reprogramming of human tumor antigen-specific T cells to hiPSC followed by redifferentiation to T cell lineage has the potential to produce rejuvenated tumor antigen-specific T cells. Described here is a method for generating tumor antigen-specific CD8αβ+ single positive (SP) T cells from hiPSC using OP9/DLL1 co-culture system. This method is a powerful tool for in vitro T cell lineage generation and will facilitate the development of in vitro derived T cells for use in regenerative medicine and cell-based therapies.

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          Author and article information

          Journal
          J Vis Exp
          Journal of visualized experiments : JoVE
          MyJove Corporation
          1940-087X
          1940-087X
          October 24 2019
          : 152
          Affiliations
          [1 ] Surgery Branch, National Cancer Institute, NIH; Center for Cell-Based Therapy, National Cancer Institute, NIH.
          [2 ] Surgery Branch, National Cancer Institute, NIH; Center for Cell-Based Therapy, National Cancer Institute, NIH; vizcardo@nih.gov.
          [3 ] Surgery Branch, National Cancer Institute, NIH.
          [4 ] Laboratory of Immunology, Institute for Frontier Life and Medical Sciences, Kyoto University.
          Article
          10.3791/59997
          31710026
          99f835a8-37e7-4531-bae4-b9b7f1d3df92
          History

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