Generation of chimeric antigen receptor-macrophages by using human induced pluripotent stem cells

被引:0
|
作者
Kitajima, Kenji [1 ]
Hara, Takahiko [1 ,2 ,3 ]
机构
[1] Tokyo Metropolitan Inst Med Sci, Stem Cell Project, Tokyo, Japan
[2] Tokyo Med & Dent Univ, Grad Sch Med & Dent Sci, Tokyo, Japan
[3] Tokyo Metropolitan Univ, Grad Sch Sci, Dept Biol Sci, Tokyo, Japan
关键词
TARGET; BLOOD;
D O I
10.1016/j.bbrc.2024.151158
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Cancer immunotherapy using chimeric antigen receptor (CAR) cells shows high therapeutic efficacy against several types of leukemia. Among acute lymphoblastic leukemias (ALLs), B cell-derived ALL can be cured by CAR-expressing T cells (CAR-Ts); however, CAR-T cells cannot be simply applied for T cell-derived ALL because antigens expressed by T-ALL cells, but not by CAR-T cells, have not yet been identified. To apply CAR-T therapy for T-ALL, gene editing of CAR required to avoid attacking CAR-T cells themselves. Alternatively, CAR-expressing macrophages (CAR-Ms) have proven to be effective against various suggesting that CAR-Ms may also be effective against T-ALL. Recently, we developed an efficient differentiation induction system to generate a large number macrophages from human induced pluripotent stem cells (iPSCs). Here, we asked whether these human iPSC-derived macrophages (iPS-MACs) can be develop and evaluate CAR-based immunotherapy against T-ALLs. When non-transduced iPS-MACs were co-cultured with human T-ALL-derived cells, the appeared to phagocytose parts of T-ALL cells; this method of phagocytosis operated mainly through incorporation of small, "bite-sized" vesicles derived from ALL cells into iPS-MACs (similar to trogocytosis). By contrast, when CAR-expressing iPS-MACs were co-cultured with T-ALL cells, iPS-MACs engulfed the whole cell. Thus, our differentiation induction system may be a promising tool for building up CAR-M therapy for T-ALLs.
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页数:7
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