標題: Pharmacologically upregulated carcinoembryonic antigen-expression enhances the cytolytic activity of genetically-modified chimeric antigen receptor NK-92MI against colorectal cancer cells
作者: Shiozawa, Masayuki
Chang, Chuan-Hsin
Huang, Yi-Chun
Chen, Yi-Ching
Chi, Mau-Shin
Hao, Hsu-Chao
Chang, Yue-Cune
Takeda, Satoru
Chi, Kwan-Hwa
Wang, Yu-Shan
分子醫學與生物工程研究所
Institute of Molecular Medicine and Bioengineering
關鍵字: Natural killer cell;NK-92MI;Chimeric antigen receptor (CAR);Carcinoembryonic antigen (CEA);Cellular immunotherapy
公開日期: 3-Aug-2018
摘要: Background: The natural killer cell line, NK-92MI, is cytotoxic against various types of cancer. The aim of this study was to develop chimeric antigen receptor-modified (CAR) NK-92MI cells targeting carcinoembryonic antigen-expressing (CEA) tumours and increase killing efficacy by pharmacologically modifying CEA-expression. Result: We generated anti-CEA-CAR NK-92MI cells by retroviral vector transduction. This genetically-modified cell line recognised and lysed high CEA-expressing tumour cell lines (LS174T) at 47.54 +/- 12.60% and moderate CEA-expressing tumour cell lines (WiDr) at 31.14 +/- 16.92% at a 5:1 effector: target (E/T) ratio. The cell line did not lyse low CEA-expressing tumour cells (HCT116) as they did their parental cells (NK-92MI cells). The histone deacetylase-inhibitor (HDAC) sodium butyrate (NaB) and the methylation-inhibitor 5-azacytidine (5-AZA), as epigenetic modifiers, induced CEA-expression in HCT116 and WiDr cells. Although the IC50 of 5 fluorouracil (5-FU) increased, both cell lines showed collateral sensitivity to anti-CEA-CAR NK-92MI cells. The cytolytic function of anti-CEA-CAR NK-92MI cells was increased from 22.99 +/- 2.04% of lysis background to 69.20 +/- 11.92% after NaB treatment, and 69.70 +/- 9.93% after 5-AZA treatment, at a 10:1 UT ratio in HCT116 cells. The WiDr cells showed similar trend, from 22.99 +/- 4.01% of lysis background to 70.69 +/- 10.19% after NaB treatment, and 59.44 +/- 10.92% after 5-AZA treatment, at a 10:1 E/T ratio. Conclusions: This data indicates that the effector-ability of anti-CEA-CAR NK-92MI increased in a CEA-dependent manner. The combination of epigenetic-modifiers like HDAC-inhibitors, methylation-inhibitors, and adoptive-transfer of ex vivo-expanded allogeneic-NK cells may be clinically applicable to patients with in 5-FU resistant condition.
URI: http://dx.doi.org/10.1186/s12865-018-0262-z
http://hdl.handle.net/11536/147948
ISSN: 1471-2237
DOI: 10.1186/s12865-018-0262-z
期刊: BMC IMMUNOLOGY
Volume: 19
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