Study of proliferation ability of tumor antigen-loaded DC-CIK cells and its killing effect on hepatocarcinoma cells HepG2

doi:10.3760/cma.j.issn.1673-422X.2019.01.001

Abstract

Abstract: Objective To observe the proliferation ability of cocultured dendritic cells (DCs) loaded with tumor antigen and cytokineinduced killer cells (CIKs) and its killing effect on hepatocarcinoma cells HepG2. Methods The antigen of hepatocarcinoma cells HepG2 was prepared by repeated freezing and thawing of liquid nitrogen. Peripheral blood mononuclear cells (PBMNCs) were isolated from healthy donors by blood cell separator, then DCs and CIKs were induced. AgDCs were obtained by impinging DCs with tumor antigens. CIKs were divided into three groups: the first group was CIKs alone, the second group was mixed in the proportion of DCs∶CIKs=1∶5, and the third group was mixed in the proportion of Ag-DCs∶CIKs=1∶5. The three groups of cells were recorded as CIK group, DC-CIK group and Ag-DC-CIK group. The proliferation and cell phenotype of the three groups of cells were observed and the killing effects on hepatocarcinoma cells HepG2 were detected by methyl thiazolyl tetrazolium (MTT) assay. Results The proliferation multiples of the three groups of cells were gradually increased with the prolongation of culture time, and the proliferation rates of Ag-DC-CIK on the 9th day (61.32±1.72), the 12th day (190.83±3.53) and the 15th day (399.09±5.60) were significantly higher than those of CIK group (22.47±2.07, 55.91±1.81, 83.20±2.34) and DC-CIK group (40.26±2.49, 125.03±4.16, 251.55±3.25), and the difference between the three group was statistically significant (F=185.78, P=0.033; F=297.35, P=0.018; F=455.37, P<0.001), in addition, the differences between each two groups were statistically significant (all P＜0.05). The cytotoxicity of Ag-DC-CIK to HepG2 cells at the effective target ratios of 5∶1 (31.71%±0.29%), 10∶1 (42.43%±1.86%) and 20∶1 (57.69%±1.11%) were significantly higher than those of CIK group (12.11%±1.14%, 21.30%±0.52%, 30.71%±1.26%) and DC-CIK group (20.06%±0.67%, 29.89%±1.37%, 39.11%±0.92%), and the difference between the three group was statistically significant (F=159.64, P=0.037; F=199.36, P=0.025; F=302.08, P＜0.001), in addition, the differences between each two groups were statistically significant (all P＜0.05). On the 15th day of cell culture, the flow cytometry analysis showed that all the three groups were expressed CD3+CD8+, CD3+CD56+ double positive cells, the contents of CD3+CD8+、CD3+CD56+ double positive cells in the Ag-DC-CIK group (88.12%±1.24%, 61.35%±2.63%) were significantly higher than those in the CIK group (54.37%±3.08%, 18.22%±1.83%) and DC-CIK group (69.80%±1.46%, 39.51%±2.17%), and the difference between the three group was statistically significant (F=414.32, P<0.001; F=378.60, P<0.001), in addition, the differences between each two groups were statistically significant (all P＜0.001). Conclusion The proliferation ability and killing effect of Ag-DC-CIK that obtained from antigen pulsed DCs cocultured with CIKs are significantly higher than those of CIKs and DCCIKs.

Key words: Dendritic cells, Killer cells, Cell line, tumor

References

［1］ Bai K, Cao Y, Huang Q, et al. Prognostic value of Ki67 expression for patients with surgically resected hepatocellular carcinoma: perspectives from a high incidence area［J］. Clin Lab, 2017, 63(2): 355-364. DOI: 10.7754/Clin.Lab.2016.160638. ［2］ Cheng XY, Li JL. Biological activity of cytotoxic dendritic cells cocultured with cytokineinduced killer cells and their effect on acute leukemia cells［J］. Genet Mol Res, 2015, 14(4): 13208-13214. DOI: 10.4238/2015.October.26.17. ［3］谭斌, 朱丹, 张长法, 等. DC联合CIK细胞治疗对中晚期肝癌患者免疫功能及生活质量的影响［J］. 当代医学, 2015, 21(26): 64-65. DOI: 10.3969/j.issn.1009-4393.2015.26.042. ［4］张蒿, 王恩忠, 白春学, 等. 共培养的树突状细胞与CIK细胞的体外增殖和杀瘤活性研究［J］. 实验生物学报, 2003, 36(5): 375-380. ［5］ Xin G, Schauder DM, Jing W, et al. Pathogen boosted adoptive cell transfer immunotherapy to treat solid tumors［J］. Proc Natl Acad Sci U S A, 2017, 114(4): 740-745. DOI: 10.1073/pnas.1614315114. ［6］ Steinman RM, Cohn ZA. Identification of a novel cell type in peripheral lymphoid organs of mice. I. Morphology, quantitation, tissue distribution［J］. J Exp Med, 1973, 137(5): 1142-1162. ［7］ SchmidtWolf IG, Lefterova P, Mehta BA, et al. Phenotypic characterization and identification of effector cells involved in tumor cell recognition of cytokineinduced killer cells［J］. Exp Hematol, 1993, 21(13): 1673-1679. ［8］ Cao J, Chen C, Wang Y, et al. Influence of autologous dendritic cells on cytokineinduced killer cell proliferation, cell phenotype and antitumor activity in vitro［J］. Oncol Lett, 2016, 12(3): 2033-2037. ［9］ Hotblack A, Seshadri S, Zhang L, et al. Dendritic cells crosspresent immunogenic lentivectorencoded antigen from transduced cells to prime functional T cell immunity［J］. Mol Ther, 2017, 25(2): 504-511. DOI: 10.1016/j.ymthe.2016.11.001. ［10］ Alaniz L, Rizzo MM, Mazzolini G. Pulsing dendritic cells with whole tumor cell lysates［J］. Methods Mol Biol, 2014, 1139: 27-31. DOI: 10.1007/978-1-4939-0345-0-3. ［11］ Jung NC, Lee JH, Choi HJ, et al. Dendritic cell immunotherapy combined with cytokineinduced killer cells effectively suppresses established hepatocellular carcinomas in mice［J］. Immunol Invest, 2016, 45(6): 553-565. DOI: 10.1080/08820139.2016.1183025. ［12］ Mrten A, Ziske C, Schttker B, et al. Interactions between dendritic cells and cytokineinduced killer cells lead to an activation of both populations［J］. J Immunother, 2001, 24(6): 502-510. ［13］ Mrten A, Renoth S, von LilienfeldToal M, et al. Enhanced lytic activity of cytokineinduced killer cells against multiple myeloma cells after coculture with idiotypepulsed dendritic cells［J］. Haematologica, 2011, 86(10): 1029-1037.

[1]	Miao Nana, Tu Wenyong, Kong Yuehong, Wang Xu, Xu Xuanli. Effect of ionizing radiation on the NKG2D ligand expression on the tumor cell SCC25 surface and the killing effect on tumor cells [J]. Journal of International Oncology, 2017, 44(8): 561-564.
[2]	LUO Cong, TAO Ning. Chemotherapy and tumor immunogenic cell death [J]. Journal of International Oncology, 2017, 44(5): 369-372.
[3]	陈邓林，陈俊民. 6-sulfo-LacNAc dendritic cells and tumors [J]. Journal of International Oncology, 2017, 44(11): 834-837.
[4]	WANG Xiao-Bo, WU Di-Jun, CHEN Wei-Ping, LIU Jian. Influence of radiotherapy on the immune function and prognosis of patients with esophageal cancer [J]. Journal of International Oncology, 2016, 43(12): 886-891.
[5]	ZHANG Zhi-Sheng. Effect of DCCIK combined with chemotherapy on Treg cell expression and prognosis in patients with breast cancer [J]. Journal of International Oncology, 2016, 43(12): 881-885.
[6]	Wang Peng, Luan Zhiyong, Liu Junquan, Hang Min， Pan Jin, Zhang Nanzheng. Effects of DC loaded α-GalCer combined with tumor specific cytotoxic T lymphocytes on the growth of transplanted Heps hepatoma in mice [J]. Journal of International Oncology, 2016, 43(11): 806-811.
[7]	Xue Kewei, Li Guixin, Li Xinxin, Guo Yingxue, Li Ao, Wang Wenhao. Effect of umbilical cord blood dendritic cells induced by gastric cancer antigen combined with CIK cells in gastric cancer cell lines SGC-7901 [J]. Journal of International Oncology, 2015, 42(7): 485-487.
[8]	Xue Ming, Guo Mingkun. Effect of adoptive immunotherapy with CIK cells combined with interleukin-2 on immunologic function and life qualities of patients with nonsmall cell lung cancer [J]. Journal of International Oncology, 2015, 42(2): 88-90.
[9]	DAN Chan-Chan, SHI Liang-Rong, DING Mei-Qian, ZHU Yi-Bei, XU Bin, JIANG Jing-Ting, WU Chang-Ping. The research of antitumor activities in vitro of DCs loading antigen prouced by radiofrequency ablation of tumor combined with CIK cells [J]. Journal of International Oncology, 2014, 41(6): 471-475.
[10]	WANG Yue, YU Jin-Pu, REN Xiu-Bao. Mechanisms of STAT family mediated IDO regulation in dendritic cells [J]. Journal of International Oncology, 2013, 40(3): 163-165.
[11]	WANG Wen-Hao, LI Gui-Xin, LIU Jin. Assessment of CIK cells in adoptive cellular therapy [J]. Journal of International Oncology, 2013, 40(2): 106-108.
[12]	SHANG Yi-Man, WANG Zi-Bing, MA Yi-Jie, ZHANG Yong, GAO Quan-Li. Adoptive cellular immunotherapy for cancer [J]. Journal of International Oncology, 2013, 40(2): 103-106.
[13]	GAO Meng, YUN Sheng. Functions of cytokine induced killer cells in oncotherapy [J]. Journal of International Oncology, 2013, 40(12): 908-911.
[14]	QIU Hui, ZHANG Jun-Ping. Research progress of anti-tumor effect of the modified DC vaccine [J]. Journal of International Oncology, 2013, 40(1): 21-24.
[15]	WANG Chun-hua. Anti-tumor mechanism of CIK cells and research [J]. Journal of International Oncology, 2012, 39(5): 348-351.