佛波酯诱导低剂量美法仑处理的MOPC - 315肿瘤荷瘤小鼠脾脏CD8⁺ T细胞溶解活性增强。
Phorbol ester-induced enhancement in lytic activity of CD8+ splenic T cells from low-dose melphalan-treated MOPC-315-tumor bearers.
作者信息
Weiskirch L M, Baumgartel B A, Barker E, Mokyr M B
机构信息
Department of Microbiology and Immunology, University of Illinois, Chicago 60680.
出版信息
Cancer Immunol Immunother. 1991;32(6):353-63. doi: 10.1007/BF01741330.
We have previously shown that while spleen cells from untreated mice bearing a large MOPC-315 tumor are not cytotoxic in vitro for MOPC-315 tumor cells, spleen cells obtained from such mice on day 7 after low-dose melphalan (L-phenylalanine mustard); L-PAM therapy exert a substantial anti-MOPC-315 cytotoxicity [Mokyr et al. (1989) Cancer Res 49: 4597]. Here we show that this anti-MOPC-315 lytic activity is evident by day 5, and peaks on day 7 after the low-dose chemotherapy, at a time when the mice are actively engaged in tumor eradication. Short-term exposure of spleen cells from mice bearing a MOPC-315 tumor and treated with low-dose L-PAM (L-PAM TuB mice) to phorbol 12-myristate 13-acetate (PMA) was found to enhance greatly the ability of these spleen cells to lyse MOPC-315 tumor cells. The highest level of anti-MOPC-315 cytotoxicity was obtained when spleen cells from tumor-bearing mice that had received chemotherapy 7 days earlier were exposed to PMA at a concentration of 1-10 ng/ml. The exertion of the enhanced anti-MOPC-315 lytic activity by L-PAM TuB spleen cells exposed to PMA was found to require CD8+, but not CD4+, T cells. The apparent specificity of the lytic activity exerted by the PMA-stimulated L-PAM TuB spleen cells was illustrated not only by the inability of the spleen cells to lyse an allogeneic, antigenically unrelated thymoma (EL4), but also by their relatively weak lytic activity for two antigenically related syngeneic plasmacytomas. In addition, when EL4 target cells were admixed with MOPC-315 tumor cells, the lytic activity triggered in the L-PAM TuB spleen cells by the MOPC-315 tumor cells plus PMA was not effective in lysing the antigenically unrelated target cells. Moreover, even in the presence of the calcium-specific ionophore, ionomycin, L-PAM TuB spleen cells exposed to PMA were unable to lyse the EL4 target cells. Thus, fresh CD8+ splenic T cells from L-PAM TuB mice that are in the process of eradicating a large MOPC-315 tumor as a consequence of low-dose L-PAM therapy can be triggered with PMA to exert enhanced lytic activity against MOPC-315 tumor cells.(ABSTRACT TRUNCATED AT 400 WORDS)
我们之前已经表明,虽然携带大型MOPC - 315肿瘤的未治疗小鼠的脾细胞在体外对MOPC - 315肿瘤细胞没有细胞毒性,但在低剂量美法仑(L - 苯丙氨酸氮芥;L - PAM)治疗7天后从这些小鼠获得的脾细胞具有显著的抗MOPC - 315细胞毒性[莫基尔等人(1989年)《癌症研究》49: 4597]。在此我们表明,这种抗MOPC - 315裂解活性在低剂量化疗后第5天就很明显,并在第7天达到峰值,此时小鼠正在积极清除肿瘤。发现携带MOPC - 315肿瘤并用低剂量L - PAM治疗的小鼠(L - PAM TuB小鼠)的脾细胞短期暴露于佛波醇12 - 肉豆蔻酸酯13 - 乙酸酯(PMA)可极大地增强这些脾细胞裂解MOPC - 315肿瘤细胞的能力。当7天前接受化疗的荷瘤小鼠的脾细胞暴露于浓度为1 - 10 ng/ml的PMA时,获得了最高水平的抗MOPC - 315细胞毒性。发现暴露于PMA的L - PAM TuB脾细胞发挥增强的抗MOPC - 315裂解活性需要CD8 + 而非CD4 + T细胞。PMA刺激的L - PAM TuB脾细胞发挥的裂解活性的明显特异性不仅体现在脾细胞无法裂解同种异体、抗原无关的胸腺瘤(EL4),还体现在它们对两种抗原相关的同基因浆细胞瘤的裂解活性相对较弱。此外,当EL4靶细胞与MOPC - 315肿瘤细胞混合时,MOPC - 315肿瘤细胞加PMA在L - PAM TuB脾细胞中触发的裂解活性对裂解抗原无关的靶细胞无效。而且,即使在存在钙特异性离子载体离子霉素的情况下,暴露于PMA的L - PAM TuB脾细胞也无法裂解EL4靶细胞。因此,由于低剂量L - PAM治疗正在清除大型MOPC - 315肿瘤的L - PAM TuB小鼠的新鲜CD8 + 脾T细胞可以用PMA触发,以发挥对MOPC - 315肿瘤细胞增强的裂解活性。(摘要截短至400字)
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