Mitchell M S, Harel W, Kan-Mitchell J, LeMay L G, Goedegebuure P, Huang X Q, Hofman F, Groshen S
Kenneth Norris Jr. Comprehensive Cancer Center, University of Southern California, Los Angeles 90033.
Ann N Y Acad Sci. 1993 Aug 12;690:153-66. doi: 10.1111/j.1749-6632.1993.tb44005.x.
Since 1985, we have conducted clinical trials with a therapeutic melanoma vaccine (melanoma theraccine). Mechanical lysates of two melanoma cell lines chosen for their complementary characteristics were combined with the adjuvant DETOX and injected subcutaneously on weeks 1, 2, 3, 4, and 6 for one or two courses and then monthly in patients with objective clinical responses. Of 106 patients, 20 had objective clinical regression of tumor masses, 5 with complete responses. The median duration of response was 21 months. Twelve patients lived at least 2 years, with a median survival of nearly 3 years. Two of them are free of disease for > 2 and > 6 years, respectively. However, it was not necessary to achieve complete remissions to cause an increase in survival, and most of the long-surviving patients have one or more (stable) residual nodules. The pace of the disease process was clearly slowed in those individuals. A rise in the level of cytotoxic T-lymphocyte precursors in the blood (pTC) correlated with clinical response. Only those patients who had a rise in pTC had a remission. In addition to "classical" CD8+ Tc, CD4+ Tc were cloned from the blood of immunized patients. Melanoma-specific Tc of both types that killed autologous melanoma but not matched lymphoblastoid cells were detected. Allogeneic melanoma cell lines were also killed, with mainly HLA-A2/28 and HLA-B12/44/45 degenerate restriction. CD4+ Tc were restricted by HLA Class I antigens, as judged by their killing of HLA Class II-negative melanomas and blocking by anti-class I antibodies. Other CD4+ clones were blocked by both anti-HLA Class I or anti-Class II MHC monoclonal antibodies, and only two were blocked only by anti-HLA Class II. Immunohistory revealed CD4+ and CD8+ T cells in lesions under rejection, but the predominant cells were macrophages, suggesting delayed-type hypersensitivity as a possible mechanism. Clinical responses were found most often in patients with HLA-A2/28, -B12/44/45, and -C3, particularly when two or more of those alleles were present. This may have been due either to (1) similarity of MHC antigens between one of the immunizing melanomas and the patient's melanoma or (2) the intrinsic importance of these MHC molecules in presenting melanoma-associated antigens to Tc in vivo. IFN-alpha 2 b salvaged 8 of 18 patients who failed with the theraccine, regardless of MHC phenotype, perhaps through upregulation of MHC and tumor epitopes on the autochthonous tumor.
自1985年以来,我们开展了一项关于治疗性黑色素瘤疫苗(黑色素瘤治疗疫苗)的临床试验。选取了具有互补特征的两种黑色素瘤细胞系的机械裂解物,将其与佐剂DETOX混合,于第1、2、3、4和6周皮下注射,进行一或两个疗程,之后对有客观临床反应的患者每月注射一次。106例患者中,20例出现肿瘤块的客观临床消退,5例完全缓解。反应的中位持续时间为21个月。12例患者存活至少2年,中位生存期近3年。其中2例分别无病生存超过2年和6年。然而,并不需要达到完全缓解才能使生存期延长,大多数长期存活的患者有一个或多个(稳定的)残留结节。在这些个体中,疾病进程明显放缓。血液中细胞毒性T淋巴细胞前体(pTC)水平的升高与临床反应相关。只有pTC水平升高的患者出现缓解。除了“经典的”CD8⁺Tc外,还从免疫患者的血液中克隆出了CD4⁺Tc。检测到两种类型的黑色素瘤特异性Tc,它们能杀死自体黑色素瘤细胞,但不能杀死匹配的淋巴母细胞系细胞。同种异体黑色素瘤细胞系也被杀死,主要受HLA - A2/28和HLA - B12/44/45的简并性限制。CD4⁺Tc受HLA I类抗原限制,这是通过它们对HLA II类阴性黑色素瘤的杀伤作用以及抗I类抗体的阻断作用来判断的。其他CD4⁺克隆被抗HLA I类或抗II类MHC单克隆抗体阻断,只有两个仅被抗HLA II类抗体阻断。免疫组化显示在排斥病变中有CD4⁺和CD8⁺T细胞,但主要细胞是巨噬细胞,提示迟发型超敏反应可能是一种机制。临床反应最常出现在具有HLA - A2/28、- B12/44/45和- C3的患者中,特别是当存在两个或更多这些等位基因时。这可能是由于(1)免疫用黑色素瘤之一与患者黑色素瘤之间MHC抗原的相似性,或者(2)这些MHC分子在体内将黑色素瘤相关抗原呈递给Tc方面的内在重要性。干扰素α - 2b挽救了18例使用治疗疫苗失败的患者中的8例,无论MHC表型如何,这可能是通过上调自身肿瘤上的MHC和肿瘤表位来实现的。
