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Human recombinant IL‐4 decreases the emergence of non‐specific cytolytic cells and favours the appearance of memory cells (CD4 + CD45RO + ) in the IL‐2‐driven development of cytotoxic T lymphocytes against autologous ovarian tumour cells
Author(s) -
ROTH A. D.,
DUPUIS S.,
ALBERTO P.
Publication year - 1995
Publication title -
clinical & experimental immunology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.329
H-Index - 135
eISSN - 1365-2249
pISSN - 0009-9104
DOI - 10.1111/j.1365-2249.1995.tb08365.x
Subject(s) - cytotoxic t cell , immunology , cytolysis , biology , interleukin 2 , lymphokine activated killer cell , cytotoxicity , ctl* , interleukin 15 , interleukin 12 , cytokine , interleukin , t cell , interleukin 21 , immune system , in vitro , cd8 , biochemistry
SUMMARY As IL‐4 and IL‐6 have also been reported to promote the development of T lymphocytes such as IL‐2, we investigated their role in the development of specific cytotoxic T lymphocytes (CTL) against autologous ovarian tumours in mixed lymphocyte tumour cultures (MLTC). Peripheral blood lymphocytes (PBL) from five ovarian carcinoma (OC) patients were incubated with autologous OC cells at a PBL:OC cell ratio of 20:1 in IL‐2 alone (50 U/ml for the first week and 200 U/ml thereafter) or with IL‐4 (100 U/ml) and/or IL‐6 (5 U/ml). Neither IL‐4 nor IL‐6 improved lymphocyte proliferation consistently. In contrast, IL‐4 reduced significantly the development of LAK activity as assayed against Daudi cell line, and decreased modestly the emergence of natural killer (NK) activity as assayed against K562. This property was not shared by IL‐6. The prevention of the development of non‐specific cytolytic activity (LAK and NK activities) was much stronger when the MLTC was started with IL‐4 in the absence of IL‐2 during the first week in culture. A concomitant drop in NKH‐1 expression (CD56) was observed. By inhibiting the emergence of non‐specific cytotoxicity, IL‐4 provided better evidence of the specific cytolytic activity directed at ovarian cells. In parallel, a significant increase in the generation of memory cells (CD4 + CD45RO + ) was observed with IL‐4. In conclusion, in this model, IL‐4 added before IL‐2 decreases significantly the emergence of non‐specific cytotoxic cells, and promotes the generation of memory cells. These properties may be of interest in the design of strategies aimed at obtaining tumour‐specific cells for investigational and immunotherapeutic purposes.

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