Ward B A, Shu S, Chou T, Perry-Lalley D, Chang A E
Surgery Branch, National Cancer Institute, Bethesda, MD 20892.
J Immunol. 1988 Aug 1;141(3):1047-53.
The adoptive transfer of specifically sensitized T lymphocytes can effectively mediate the regression of established local and metastatic tumors. Previous experiments using the weakly immunogenic MCA 105 sarcoma indicated that cellular interactions between transferred L3T4+ helper and Lyt-2+ cytotoxic immune T cells were necessary for mediating tumor regression. In this study, the kinetics of T-T cell interactions were analyzed by in vivo depletion of T cell subsets with mAb. The anti-tumor efficacy of transferred immune cells was abrogated by in vivo administration of either L3T4 or Lyt-2 mAb on the day of cellular therapy. However, if mAb were given 3 days after the transfer of immune cells, depletion of Lyt-2+ but not L3T4+ cells abrogated anti-tumor efficacy. T cell depletion on day 6 after transfer of immune cells had no adverse effect on tumor regression, indicating the period required for T cell reactivity in vivo. Furthermore, depletion of Ia+ cells by in vivo mAb treatment abrogated the anti-tumor efficacy of immune cells. It is thus hypothesized that there are two distinct but sequential phases of in vivo T cell interactions leading to the regression of established tumors after adoptive immunotherapy. An initial "helper/inducer" phase apparently requires the interaction of L3T4+ immune cells and the tumor Ag involving Ia+ cells. The inducement of L3T4+ cell activation is to provide helper function via the secretion of IL-2. The second phase designated as an "effector phase" involves differentiation of immune Lyt-2+ cells under the influence of IL-2 secreted during the helper/inducer phase for generation of mature Lyt-2+ effector cells. To further support the hypothesis of a two-phase process we have examined the phenotype and kinetics of tumor regression mediated by effector cells generated by secondary in vitro sensitization (IVS). Although the IVS cells were generated from fresh MCA 105 immune spleen cells, their anti-tumor efficacy was mediated solely by Lyt-2+ lymphocytes. Kinetic studies revealed that the in vivo requirement of IVS Lyt-2+ effector cells to mediate tumor regression was less than 3 days, and the anti-tumor reactivity of these cells was not affected by in vivo depletion of Ia+ cells. Thus, the IVS reaction is likely representative of the in vivo counterpart of the helper/inducer phase leading to the generation of mature Lyt-2+ immune effector cells. Tumor regression after transfer of Lyt-2+ cells generated in IVS therefore required a relatively shorter period of time than that required after the transfer of fresh noncultured MCA 105 immune spleen cells.
特异性致敏T淋巴细胞的过继转移能够有效介导已形成的局部和转移性肿瘤的消退。先前使用弱免疫原性的MCA 105肉瘤进行的实验表明,转移的L3T4 +辅助性和Lyt-2 +细胞毒性免疫T细胞之间的细胞相互作用对于介导肿瘤消退是必需的。在本研究中,通过用单克隆抗体在体内清除T细胞亚群来分析T-T细胞相互作用的动力学。在细胞治疗当天,体内给予L3T4或Lyt-2单克隆抗体可消除转移免疫细胞的抗肿瘤功效。然而,如果在免疫细胞转移后3天给予单克隆抗体,清除Lyt-2 +而不是L3T4 +细胞会消除抗肿瘤功效。免疫细胞转移后第6天的T细胞清除对肿瘤消退没有不利影响,这表明体内T细胞反应所需的时间。此外,体内单克隆抗体治疗清除Ia +细胞可消除免疫细胞的抗肿瘤功效。因此,据推测,过继免疫治疗后,体内T细胞相互作用存在两个不同但相继的阶段,导致已形成肿瘤的消退。最初的“辅助/诱导”阶段显然需要L3T4 +免疫细胞与涉及Ia +细胞的肿瘤抗原相互作用。L3T4 +细胞活化的诱导是通过分泌IL-2来提供辅助功能。第二个阶段称为“效应阶段”,涉及在辅助/诱导阶段分泌的IL-2影响下免疫Lyt-2 +细胞的分化,以产生成熟的Lyt-2 +效应细胞。为了进一步支持两阶段过程的假设,我们研究了由二次体外致敏(IVS)产生的效应细胞介导的肿瘤消退的表型和动力学。尽管IVS细胞是由新鲜的MCA 105免疫脾细胞产生的,但其抗肿瘤功效仅由Lyt-2 +淋巴细胞介导。动力学研究表明,IVS Lyt-2 +效应细胞在体内介导肿瘤消退的时间要求少于3天,并且这些细胞的抗肿瘤反应性不受体内Ia +细胞清除的影响。因此,IVS反应可能代表导致成熟Lyt-2 +免疫效应细胞产生的辅助/诱导阶段的体内对应物。因此,与新鲜未培养的MCA 105免疫脾细胞转移后相比,IVS中产生的Lyt-2 +细胞转移后肿瘤消退所需的时间相对较短。
