Saijo N, Ozaki A, Ishihara J, Sakurai M, Sasaki Y, Takahashi H, Sano T, Hoshi A
Gan To Kagaku Ryoho. 1986 Apr;13(4 Pt 2):1290-7.
There are two strategies for evaluating the antitumor effect of IL-2. In the first approach IL-2 has been used to support the proliferation of T-effector cells or LAK cells in vitro in the hope that large quantities of these effector cells can be used therapeutically. This approach has shown some efficacy in animal models if LAK cells are administered in combination with IL-2. However, it is extremely difficult to standardize the numbers of lymphocytes and the biological activity of effector cells for clinical use. Recently the cloning of IL-2 has made available large quantities of purified recombinant IL-2 (rIL-2) for preclinical and clinical trials. Accordingly there have been recent attempts at injecting rIL-2 directly to stimulate effector cells in vivo. In this study, in vivo and in vitro augmentation of the cytotoxicity of spleen lymphocytes against syngeneic B-16 melanoma cells (induction of LAK cells) and the suppression of artificial pulmonary and liver metastases of B-16 melanoma in C57BL/6 mice was tried by subcutaneous multiple injections of high-dose human rIL-2. In addition, the immunosuppressive effect of a water-soluble nitrosourea derivative (ACNU) was determined in terms of the cytotoxicity of spleen lymphocytes, and the restoring effect of lymphokine-activated killer (LAK) cells and/or human recombinant interleukin-2 (rIL-2) on the cytotoxicities of spleen lymphocytes were examined in ACNU-treated C57 BL/6 mice. It was also tested whether the administration of LAK cells and/or rIL-2 could reduce the increased numbers of pulmonary metastases in ACNU-treated mice. The cytotoxicity of spleen lymphocytes against YAC-1 cells as well as against syngeneic B-16 and F-10 melanoma cells was augmented not only by incubation of spleen lymphocytes with human recombinant interleukin-2 (rIL-2) in vitro but also by injecting high-dose rIL-2 into C57BL/6 mice for more than 3 consecutive days. In animals injected with multiple high doses of rIL-2 subcutaneously, the numbers of tumor nodules in the lung were significantly decreased 21 days after intravenous tumor inoculation. In addition, in these groups of animals no liver metastases were observed although liver metastases were detected in 6/11 of control mice. The maximum effective dose of ACNU suppressed the cytotoxicity of spleen lymphocytes and pretreatment with ACNU enhanced the induction of artificial pulmonary metastases.(ABSTRACT TRUNCATED AT 400 WORDS)
评估白细胞介素-2(IL-2)抗肿瘤效果有两种策略。第一种方法是,IL-2已被用于在体外支持T效应细胞或淋巴因子激活的杀伤细胞(LAK细胞)的增殖,希望大量的这些效应细胞可用于治疗。如果将LAK细胞与IL-2联合给药,这种方法在动物模型中已显示出一定疗效。然而,要标准化用于临床的淋巴细胞数量和效应细胞的生物活性极其困难。最近,IL-2的克隆使得大量纯化的重组IL-2(rIL-2)可用于临床前和临床试验。因此,最近有人尝试直接注射rIL-2以在体内刺激效应细胞。在本研究中,通过皮下多次注射高剂量人rIL-2,尝试在体内和体外增强C57BL/6小鼠脾脏淋巴细胞对同基因B-16黑色素瘤细胞的细胞毒性(诱导LAK细胞)以及抑制B-16黑色素瘤的人工肺和肝转移。此外,根据脾脏淋巴细胞的细胞毒性确定了水溶性亚硝基脲衍生物(ACNU)的免疫抑制作用,并在ACNU处理的C57BL/6小鼠中检测了淋巴因子激活的杀伤细胞(LAK)和/或人重组白细胞介素-2(rIL-2)对脾脏淋巴细胞细胞毒性的恢复作用。还测试了给予LAK细胞和/或rIL-2是否能减少ACNU处理小鼠中肺转移瘤数量的增加。脾脏淋巴细胞对YAC-1细胞以及对同基因B-16和F-10黑色素瘤细胞的细胞毒性不仅通过在体外将脾脏淋巴细胞与人重组白细胞介素-2(rIL-2)孵育而增强,而且通过连续3天以上向C57BL/6小鼠注射高剂量rIL-2而增强。在皮下注射多次高剂量rIL-2的动物中,静脉接种肿瘤21天后肺内肿瘤结节数量显著减少。此外,在这些动物组中未观察到肝转移,而在11只对照小鼠中有6只检测到肝转移。ACNU的最大有效剂量抑制了脾脏淋巴细胞的细胞毒性,ACNU预处理增强了人工肺转移的诱导。(摘要截短至400字)
