细胞因子基因转导到非免疫基因小鼠肿瘤细胞。

S Morecki, A Lubina-Salomon, S Slavin, A Nagler
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引用次数: 0

摘要

研究了细胞因子转导对小鼠非免疫原性乳腺癌(4T1)、急性髓系白血病(mAML)和部分免疫原性b细胞白血病(BCL1)的致瘤性和免疫原性的影响。含有GM-CSF、IL-2或ifn - γ基因的逆转录病毒载体转导对4T1乳腺肿瘤或BCL1没有显著的抗肿瘤作用。用转染了GM-CSF和IL-2基因的4T1细胞接种小鼠后,再体外暴露于重组ifn - γ,小鼠局部肿瘤大小减小,但存活时间没有延长。与接种未转导的mAML细胞相比,转染ifn - γ基因的mAML细胞的致瘤性显著降低,小鼠的存活时间延长。上述每种细胞因子的转导均不影响这些肿瘤模型细胞的免疫原性。结果表明,自发和非免疫原性实验肿瘤模型的遗传修饰不一定支持细胞因子基因治疗直接用于临床应用。为了在自发性非免疫原性恶性肿瘤中实现抗肿瘤效果,尚未建立更有效的方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cytokine gene transduction into non-immunogeneic murine tumor cells.

The effect of cytokine transduction on the tumorigenicity and immunogenicity of murine non-immunogeneic mammary carcinoma (4T1), acute myeloid leukemia (mAML) and partially immunogenic B-cell leukemia (BCL1) has been evaluated in syngeneic strains of mice. Transduction by retroviral vectors containing the genes for GM-CSF, IL-2 or IFN-gamma did not lead to a marked antitumor effect in 4T1 mammary tumor or BCL1. A reduced local tumor size was observed in mice inoculated with 4T1 cells transduced with both GM-CSF and IL-2 genes followed by an in vitro exposure to recombinant IFN-gamma, but survival was not prolonged. Tumorigenicity of mAML cells transduced with the gene coding for IFN-gamma was significantly reduced as manifested by prolonged survival of mice in comparison with animals inoculated with non-transduced mAML cells. Transduction by each of the aforementioned cytokines did not affect the immunogenicity of these tumor model cells. The results suggest that genetic modification of spontaneous and non-immunogenic experimental tumor models does not necessarily support direct utilization of cytokine gene therapy for clinical application. More effective methods have yet to be established in order to achieve an antitumor effect in spontaneous non-immunogenic malignancies.

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