@article{CJCR1642,
author = {Hulai Wei and Haixiang Su and Xiaojian Yao},
title = {BIOLOGICAL FEATURES OF HUMAN T-ACTIVATED KILLER CELLS},
journal = {Chinese Journal of Cancer Research},
volume = {11},
number = {2},
year = {2013},
keywords = {},
abstract = {Objective: To investigate the immunobiological essence of T-activated killer (T-AK) cells induced by anti-CD3 monoclonal antibody (CD3McAb) and recombinant interleukin-2 (rIL-2) co-stimulation.
Methods: The cytomorphology, phenotype and cytotoxicity of T-AK cells generated from human peripheral blood mononuclear cells (PBMC) were determined.
Results: T-AK cells were similar to activated lymphoblasts in morphology, more than 90% of T-AK cells expressed the phenotypes of Tlymphocytes (CD3+, CD8+), and 20%-50% of the cells were NK-like phenotype (CD16+, CD56+), some of them expressed IL-2 receptor (CD25+), CD38 antigen (CD38+) and MHC-II antigen (HLA-DR+) characteristic marks for the activated T lymphocytes. T-AK cells attacking targets were morphologically large volumes with granules and mainly contained CD8+ and CD56+ cells. TAK cells possessed high tumoricidal activities against NK-sensitive Ks62 cells and NK-resistant Raji cells, the cytotoxicity was composed of mainly CDaMcAbactivated CD3AK activity (-50%), IL-2 induced LAK activity (-30%), NK activity (-10%) and the activities of inhibitory factors in T-AK supernatant (-10%).
Conclusion: T-AK cells are a heterogeneous cell population consisting of mainly activated T lymphocytes and NK-like cells, the main part of T-AK cytotoxicity is the common activities of CD3AK cells and LAK cells.},
issn = {1993-0631}, url = {https://cjcr.amegroups.org/article/view/1642}
}