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Engineering artificial antigen-presenting cells to express a diverse array of co-stimulatory molecules.


ABSTRACT: To facilitate the therapeutic application of antigen-presenting cells (APCs), we have developed a cell-based artificial APC (aAPC) system by engineering K562 cells with lentiviruses to direct the stable expression and secretion of a variety of co-stimulatory molecules and cytokines. Here we report the use of a combinatorial lentiviral gene transfer approach to achieve long-term stable expression of at least seven genes in the K562 parental cell line. Expression of various combinations of genes on the aAPC enables the precise determination of human T-cell activation requirements, such that aAPCs can be tailored for the optimal propagation of T-cell subsets with specific growth requirements and distinct functions. The aAPCs support ex vivo growth and long-term expansion of functional human CD8 T cells without requiring the addition of exogenous cytokines, in contrast to the use of natural APCs. Distinct populations of T cells can be expanded with aAPCs expressing CD137L (4-1BBL) and/or CD80. Finally, the aAPCs provide an efficient platform to expand genetically modified T cells and to maintain CD28 expression on CD8 T cells. Therefore, K562-based aAPCs have therapeutic potential for adoptive immunotherapies and vaccinations.

SUBMITTER: Suhoski MM 

PROVIDER: S-EPMC3932757 | biostudies-literature | 2007 May

REPOSITORIES: biostudies-literature

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Engineering artificial antigen-presenting cells to express a diverse array of co-stimulatory molecules.

Suhoski Megan M MM   Golovina Tatiana N TN   Aqui Nicole A NA   Tai Victoria C VC   Varela-Rohena Angel A   Milone Michael C MC   Carroll Richard G RG   Riley James L JL   June Carl H CH  

Molecular therapy : the journal of the American Society of Gene Therapy 20070320 5


To facilitate the therapeutic application of antigen-presenting cells (APCs), we have developed a cell-based artificial APC (aAPC) system by engineering K562 cells with lentiviruses to direct the stable expression and secretion of a variety of co-stimulatory molecules and cytokines. Here we report the use of a combinatorial lentiviral gene transfer approach to achieve long-term stable expression of at least seven genes in the K562 parental cell line. Expression of various combinations of genes o  ...[more]

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