|本期目录/Table of Contents|

[1]郑竹影,孙艳,程静波,等.突变型P53特异性活化T细胞的诱导与扩增[J].浙江理工大学学报,2014,31-32(自科6):678-684.
 ZHENG Zhu ying,SUN Yan,CHENG Jing bo,et al.Induction and Amplification of Mutant P53 Specific Activated T Cells[J].Journal of Zhejiang Sci-Tech University,2014,31-32(自科6):678-684.
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突变型P53特异性活化T细胞的诱导与扩增()
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浙江理工大学学报[ISSN:1673-3851/CN:33-1338/TS]

卷:
第31-32卷
期数:
2014年自科6期
页码:
678-684
栏目:
(自科)生物与生命科学
出版日期:
2014-11-10

文章信息/Info

Title:
Induction and Amplification of Mutant P53 Specific Activated T Cells
文章编号:
1673-3851 (2014) 06-0678-07
作者:
郑竹影 孙艳 程静波 钱其军
1. 浙江理工大学生命科学学院新元医学与生物技术研究所, 杭州 310018;2. 第二军医大学东方肝胆外科医院病毒基因治疗实验室, 上海 200438
Author(s):
ZHENG Zhuying SUN Yan CHENG Jingbo QIAN Qijun
1. Xinyuan Institute of Medicine and Biotechnology, School of Life Science, Zhejiang SciTech University,Hangzhou 310018, China; 2.Laboratory of Virus and Gene Therapy, Eastern Hepatobiliary Surgical Hospital,Second Military University, Shanghai 200438, China
关键词:
多因子诱导 树突状细胞 特异性活化T细胞 扩增
分类号:
R392.12
文献标志码:
A
摘要:
采用多种细胞因子诱导外周血单核细胞分化为成熟的树突状细胞(DC,Dentritic Cell),将成熟DC与初始T细胞共培养,并连续加入DC刺激从而避免活化的T细胞凋亡。将活化的T细胞转入包被有CD3和CD28抗体的板中,使活化T细胞进一步大量扩增。流式检测多因子诱导后DC表型发现,高表达CD83、CD11c、CD11b、CD80、CD86、CCR7、CD54,低表达CD14、CD3、CD33,说明因子成功诱导单核细胞为成熟DC。流式检测扩增的活化T细胞发现高表达CD3、CD8,含有很低量的调节性T细胞(Treg),分泌大量的IFN γ,表明扩增出的细胞中活化T的含量很高,为临床研究提供参考。

参考文献/References:

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备注/Memo

备注/Memo:
收稿日期: 2014-02-22
基金项目: 上海细胞治疗工程技术研究中心,上海工程技术研究中心课题(12DZ2251600)
作者简介: 郑竹影(1988-),女,江苏无锡人,硕士研究生,研究方向为肿瘤细胞治疗
通信作者: 钱其军,E-mail:qianqj@163.com
更新日期/Last Update: 2014-11-19