Preliminary study on the cooperation of IL-6 and mB7-1 in the induction of effective antitumor immunityin vitro |
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Authors: | Qu Shen Liu Ranyi Wang Yuzhe Wang Jianbo |
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Affiliation: | (1) Department of Biochemistry, School of Basic Medical Sciences, Tongji Medical University, 430030 Wuhan |
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Abstract: | Summary To find a new way for gene therapy against tumors with weak immunogenicity, the effect of mB7-1 costimulation alone, or combined with IL-6, in inducing antitumor immunityin vitro was investigated. It was found that mB7-1 cD-NA transfected B16 cells (B16-mB7-1) induced the expansion of effector lymphocytes and the generation of specific lytic activity more effectively than wild type B16 melanoma cells (B16-wt) or mock-transfected B16 cells (B16-neo) did. (P < 0. 01), IL-6 could effectively stimulate lymphocytes proliferation, but failed to enhance its cytotoxicity, while the combination of mB7-1 and IL-6 increased both lymphocyte proliferative response and T-cell-mediated cytotoxicity more significantly than B7-1 or IL-6 did alone (P<0. 01). It was inferred that the costimulatory molecule B7-1 is required for the activation and proliferation of T lymphocytes; the expression of mB7-1 in tumor cells could increase their immunogenicity and induce effective antitumor immune response, and the combination of B7-1 and IL-6 could induce more effective antitumor immunity, indicating that cooperation of IL-6 and mB7-1 plays a role in T lymphocyte activation. This project was supported by a grant from National Educational Committee Foundation of China (No. JW 9312). |
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Keywords: | B7-1 (CD80) interleukin-6 B16 melanoma tumor /gene therapy |
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