Lafreniere R, Rosenberg S A
Cancer Res. 1985 Aug;45(8):3735-41.
Lymphokine-activated killer (LAK) cells are generated in vitro by the incubation of normal murine splenocytes in interleukin 2. We have shown previously that the systemic injection of LAK cells in conjunction with recombinant interleukin 2 can reduce the number of established pulmonary metastases in mice. In an attempt to study this approach in the treatment of hepatic metastases, we developed a technique for the induction of hepatic metastases in mice based on the intrasplenic injection of tumor cells and have tested the effects of LAK cells and recombinant interleukin 2 produced in Escherichia coli (RIL-2) therapy on these metastases. Treatment with LAK cells alone in 14 consecutive experiments rarely produced significant reduction in metastases over control (mean percentage reduction, 12%). Therapy with RIL-2 alone produced a dose-dependent reduction in the number of liver metastases. In 20 consecutive experiments when RIL-2 was administered i.p. three times a day at doses varying from 1,000 to 5,000, 10,000 to 15,000, and 25,000 units, a statistically significant (P less than 0.05) reduction in liver metastases was seen in 2 of 12, 2 of 4, and 8 of 12 determinations, respectively (percentage reduction, 0 to 97; mean, 42%). At doses greater than 25,000 units, the reduction in metastases was highly reproducible (percentage reduction, 66 to 95; mean, 83%) and was statistically significant in 14 of 14 determinations. When LAK cells were given i.v. in addition to RIL-2 administration in 16 consecutive experiments, the percentage reduction in liver metastases was markedly increased over that seen with RIL-2 alone (mean percentage reduction, 77% at doses of 5,000 to 25,000 units of RIL-2 and mean reduction, 97% for doses greater than 25,000 units of RIL-2). At doses of 5,000, 10,000, 25,000, and greater than 25,000 units of RIL-2 plus LAK cells, significant reduction of liver metastases (P less than 0.05) was achieved in 3 of 7, 2 of 2, 8 of 8, and 6 of 6 determinations, respectively. When animals were given fresh splenocytes or splenocytes cultured in complete medium without RIL-2 instead of LAK cells, no reduction in liver metastases was seen except for that attributable to the administration of RIL-2 alone. Sublethal total body irradiation of the mice prior to therapy abrogated the therapeutic effects of RIL-2, but the effects of treatment with LAK cells plus RIL-2 were maintained. Thus, treatment with RIL-2 alone or in combination with LAK cells is effective in reducing the number of established hepatic micrometastases in a murine model.(ABSTRACT TRUNCATED AT 400 WORDS)
淋巴因子激活的杀伤(LAK)细胞是通过在白细胞介素2中孵育正常小鼠脾细胞在体外产生的。我们之前已经表明,全身注射LAK细胞并联合重组白细胞介素2可以减少小鼠体内已形成的肺转移瘤数量。为了研究这种方法在治疗肝转移中的应用,我们开发了一种基于脾内注射肿瘤细胞诱导小鼠肝转移的技术,并测试了LAK细胞和大肠杆菌产生的重组白细胞介素2(RIL-2)疗法对这些转移瘤的影响。在14个连续实验中,单独用LAK细胞治疗与对照组相比很少能使转移瘤显著减少(平均减少百分比为12%)。单独用RIL-2治疗可使肝转移瘤数量呈剂量依赖性减少。在20个连续实验中,当每天腹腔注射RIL-2三次,剂量分别为1000至5000、10000至15000和25000单位时,在12次测定中有2次、4次测定中有2次以及12次测定中有8次观察到肝转移瘤有统计学意义(P小于0.05)的减少(减少百分比为0至97;平均值为42%)。在剂量大于25000单位时,转移瘤的减少具有高度可重复性(减少百分比为66至95;平均值为83%),并且在14次测定中有14次具有统计学意义。在16个连续实验中,除了给予RIL-2外还静脉注射LAK细胞时,肝转移瘤的减少百分比比单独使用RIL-2时显著增加(在RIL-2剂量为5000至25000单位时平均减少百分比为77%,在RIL-2剂量大于25000单位时平均减少97%)。在RIL-2剂量为5000、10000、2五万和大于25000单位加LAK细胞时,在7次测定中有3次、2次测定中有2次、8次测定中有8次以及6次测定中有6次分别实现了肝转移瘤的显著减少(P小于0.05)。当给动物注射新鲜脾细胞或在无RIL-2的完全培养基中培养的脾细胞而非LAK细胞时,除了单独给予RIL-2所导致酌减少外,未观察到肝转移瘤的减少。在治疗前对小鼠进行亚致死性全身照射消除了RIL-2的治疗效果,但LAK细胞加RIL-2的治疗效果得以维持。因此,单独用RIL-2或与LAK细胞联合治疗在减少小鼠模型中已形成的肝微转移瘤数量方面是有效的。(摘要截短至400字)
