Deckers P J, Pardridge D H, Wang B S, Mannick J A
Cancer Res. 1976 Oct;36(10):3690-4.
Two antigenically distinct fibrosarcomas, designated BP-8 and BP-9, induced in syngeneic C3H/HeN mice by 3,4-benzo(a)pyrene were used to study tumor-specific immunity, concomitant tumor immunity and the effect of large tumor volumes on the loss of immunological reactivity. Two groups of mice were immunized to the BP-8 tumor by amputation of growing BP-8 isografts. One group was rechallenged with the BP-8 cells, and tumor growth was not noted. Both groups of mice then received an inoculum of BP-9 cells that grew to palpable tumors to the same extent as in control mice. BP-8-immunized mice bearing progressively larger PB-9 tumors were sacrified at varying intervals after the BP-9 isograft. Tumor weight was recorded as a percentage of total body weight and viable spleen cells from these animals were tested in vitro for cytotoxicity against BP-8 and BP-9 cells in the [125I]iododeoxyuridine microcytotoxicity assay. Spleen cells from untreated mice were used as controls. The mice with growing BP-9 tumors developed an immune reaction against the tumor antigens which increased with time from initial tumor isograft and with increasing tumor size up to a definite but variable limit. Cytotoxicity to BP-9 cells rose from 18% when the BP-9 tumor was not palpable to a maximum of 77% when the tumor represented 5 to 10% of the total body weight. Cytotoxicity to BP-9 fell progressively as tumor size exceeded 15% of the total body weight and approached the 10% background cytotoxicity of control lymphocytes to BP-9 cells, when the tumor weight achieved 25% of the animal's weight. Conversely, cytotoxicity of lymphocytes against the BP-8 tumor did not vary significantly and remained about 41 to 44% over the same interval even while specific reactivity to BP-9 cells significantly decreased. In addition, with time, lymphocyte-mediated cytotoxicity to the BP-8 tumor increased from 41 to 70% if the BP-8-immunized mice had been rechallenged with antigenically identical BP-8 cells prior to the BP-9 isograft. These data suggest that loss of immunoreactivity at large tumor volumes is tumor and, presumably, antigen specific. No evidence of a generalized immune paralysis was demonstrated, since the mice always maintained immunity to the BP-8 tumor despite progressive and lethal growth of the antigenically distinct BP-9 tumor.
用3,4-苯并(a)芘在同基因C3H/HeN小鼠中诱导产生的两种抗原性不同的纤维肉瘤,分别命名为BP-8和BP-9,用于研究肿瘤特异性免疫、伴随肿瘤免疫以及大肿瘤体积对免疫反应性丧失的影响。两组小鼠通过切除生长中的BP-8同基因移植瘤对BP-8肿瘤进行免疫。一组用BP-8细胞再次攻击,未观察到肿瘤生长。然后两组小鼠都接种BP-9细胞,其生长到可触及肿瘤的程度与对照小鼠相同。在接种BP-9同基因移植瘤后的不同时间间隔,处死携带逐渐增大的BP-9肿瘤的BP-8免疫小鼠。记录肿瘤重量占总体重的百分比,并在[125I]碘脱氧尿苷微细胞毒性试验中,体外检测这些动物的活脾细胞对BP-8和BP-9细胞的细胞毒性。未处理小鼠的脾细胞用作对照。生长BP-9肿瘤的小鼠对肿瘤抗原产生免疫反应,该反应从最初的肿瘤同基因移植开始随时间增加,并随肿瘤大小增加,直至达到一个确定但可变的限度。对BP-9细胞的细胞毒性从BP-9肿瘤不可触及的时候的18%上升到肿瘤占总体重5%至10%时的最高77%。当肿瘤大小超过总体重的15%且肿瘤重量达到动物体重的25%时,对BP-9的细胞毒性逐渐下降,并接近对照淋巴细胞对BP-9细胞10%的背景细胞毒性。相反,淋巴细胞对BP-8肿瘤的细胞毒性没有显著变化,在相同时间段内保持在约41%至44%,即使对BP-9细胞的特异性反应性显著降低。此外,如果在接种BP-9同基因移植瘤之前,对BP-8免疫小鼠用抗原相同的BP-8细胞再次攻击,随着时间推移,淋巴细胞介导的对BP-8肿瘤的细胞毒性从41%增加到70%。这些数据表明,大肿瘤体积时免疫反应性的丧失是肿瘤特异性的,大概也是抗原特异性的。没有证据表明存在全身性免疫麻痹,因为尽管抗原性不同的BP-9肿瘤进行性致命生长,但小鼠始终对BP-8肿瘤保持免疫。
