Mulé J J, Shu S, Rosenberg S A
J Immunol. 1985 Jul;135(1):646-52.
We showed previously that adoptive immunotherapy with the combination of LAK cells and recombinant IL 2 (RIL 2) can markedly reduce pulmonary micrometastases from multiple sarcomas established 3 days after the i.v. injection of syngeneic tumor cells in C57BL/6 mice. In this report, we analyzed the factors required for successful therapy. Titration analysis in vivo revealed an inverse relationship between the number of pulmonary metastases remaining after treatment and both the number of LAK cells and the amount of RIL 2 administered. Fresh or unstimulated splenocytes had no anti-tumor effect; a 2- to 3-day incubation of splenocytes in RIL 2 was required. LAK cells generated from allogeneic DBA (H-2d) splenocytes were as effective in vivo as syngeneic, C57BL/6 (H-2b) LAK cells. The anti-metastatic capacity of LAK cells was significantly reduced or eliminated when irradiated with 3000 rad before adoptive transfer. The combined therapy of LAK cells plus RIL 2 was shown to be highly effective in mice immunosuppressed by 500 rad total body irradiation and in treating macrometastases established in the lung 10 days after the i.v. injection of sarcoma cells. Further, reduction of both micrometastases and macrometastases could also be achieved by RIL 2 alone when administered at higher levels than were required with LAK cells. The value of LAK cell transfer and of IL 2 administration for the treatment of tumors established at other sites is currently under investigation.
我们先前已表明,用淋巴因子激活的杀伤细胞(LAK细胞)与重组白细胞介素2(RIL-2)联合进行过继性免疫治疗,可显著减少C57BL/6小鼠静脉注射同基因肿瘤细胞3天后形成的多种肉瘤的肺微转移灶。在本报告中,我们分析了成功治疗所需的因素。体内滴定分析显示,治疗后残留的肺转移灶数量与LAK细胞数量及所给予的RIL-2量呈反比。新鲜的或未受刺激的脾细胞没有抗肿瘤作用;脾细胞需要在RIL-2中孵育2至3天。由同种异体DBA(H-2d)脾细胞产生的LAK细胞在体内与同基因的C57BL/6(H-2b)LAK细胞一样有效。LAK细胞在过继转移前用3000拉德照射后,其抗转移能力显著降低或消除。LAK细胞加RIL-2的联合疗法在经500拉德全身照射免疫抑制的小鼠以及治疗静脉注射肉瘤细胞10天后在肺中形成的大转移灶方面显示出高效。此外,当给予比与LAK细胞联合使用时所需剂量更高的RIL-2时,单独使用RIL-2也可减少微转移灶和大转移灶。目前正在研究LAK细胞转移和给予IL-2对治疗在其他部位形成的肿瘤的价值。
