Expression of chimeric antigen receptors in natural killer cells with a regulatory-compliant non-viral method

被引:0
|
作者
L Li
L N Liu
S Feller
C Allen
R Shivakumar
J Fratantoni
L A Wolfraim
H Fujisaki
D Campana
N Chopas
S Dzekunov
M Peshwa
机构
[1] MaxCyte Inc,Departments of Oncology and Pathology
[2] St Jude Children's Research Hospital,undefined
来源
Cancer Gene Therapy | 2010年 / 17卷
关键词
NK cells; chimeric antigen receptor; electroporation; non-viral; transfection; mRNA;
D O I
暂无
中图分类号
学科分类号
摘要
Natural killer (NK) cells hold promise for cancer therapy. NK cytotoxicity can be enhanced by expression of chimeric antigen receptors that re-direct specificity toward target cells by engaging cell surface molecules expressed on target cells. We developed a regulatory-compliant, scalable non-viral approach to engineer NK cells to be target-specific based on transfection of mRNA encoding chimeric receptors. Transfection of eGFP mRNA into ex vivo expanded NK cells (N=5) or purified unstimulated NK cells from peripheral blood (N=4) resulted in good cell viability with eGFP expression in 85±6% and 86±4%, 24 h after transfection, respectively. An mRNA encoding a receptor directed against CD19 (anti-CD19-BB-z) was also transfected into NK cells efficiently. Ex vivo expanded and purified unstimulated NK cells expressing anti-CD19-BB-z exhibited enhanced cytotoxicity against CD19+ target cells resulting in ⩾80% lysis of acute lymphoblastic leukemia and B-lineage chronic lymphocytic leukemia cells at effector target ratios lower than 10:1. The target-specific cytotoxicity for anti-CD19-BB-z mRNA-transfected NK cells was observed as early as 3 h after transfection and persisted for up to 3 days. The method described here should facilitate the clinical development of NK-based antigen-targeted immunotherapy for cancer.
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页码:147 / 154
页数:7
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