Castelli C, Rivoltini L, Andreola G, Carrabba M, Renkvist N, Parmiani G
Unit of Immunotherapy of Human Tumors, Istituto Nazionale Tumori, Milan, Italy.
J Cell Physiol. 2000 Mar;182(3):323-31. doi: 10.1002/(SICI)1097-4652(200003)182:3<323::AID-JCP2>3.0.CO;2-#.
In this review, we summarize the significant progress that has been made in the identification of melanoma-associated antigens (MAA) recognized by cytotoxic T-lymphocytes (CTL). These antigens belong to three main groups: tumor-associated testis-specific antigens (e.g. , MAGE, BAGE, and GAGE); melanocyte differentiation antigens (e.g., tyrosinase, Melan-A/MART-1); and mutated or aberrantly expressed molecules (e.g, CDK4, MUM-1, beta-catenin). Although strong CTL activity may be induced ex vivo against most of these antigens, often in the presence of excess cytokines and antigen, a clear understanding of the functional status of CTL in vivo and their impact on tumor growth, is still lacking. Several mechanisms are described that potentially contribute to tumor cell evasion of the immune response, suggesting that any antitumor efficacy achieved by immune effectors may be offset by factors that result ultimately in tumor progression. Nevertheless, most of these MAA are currently being investigated as immunizing agents in clinical studies, the conflicting results of which are reviewed. Indeed, the therapeutic potential of MAA has still to be fully exploited and new strategies have to be found in order to achieve an effective and long-lasting in vivo immune control of melanoma growth and progression.
在本综述中,我们总结了在识别细胞毒性T淋巴细胞(CTL)所识别的黑色素瘤相关抗原(MAA)方面取得的重大进展。这些抗原主要分为三类:肿瘤相关的睾丸特异性抗原(如MAGE、BAGE和GAGE);黑素细胞分化抗原(如酪氨酸酶、Melan-A/MART-1);以及突变或异常表达的分子(如CDK4、MUM-1、β-连环蛋白)。尽管在体外针对大多数这些抗原通常在存在过量细胞因子和抗原的情况下可诱导强烈的CTL活性,但仍缺乏对CTL在体内的功能状态及其对肿瘤生长影响的清晰认识。描述了几种可能导致肿瘤细胞逃避免疫反应的机制,这表明免疫效应器所实现的任何抗肿瘤功效可能会被最终导致肿瘤进展的因素所抵消。然而,目前大多数这些MAA正在临床研究中作为免疫制剂进行研究,并对其相互矛盾的结果进行了综述。事实上,MAA的治疗潜力仍有待充分挖掘,必须找到新的策略,以实现对黑色素瘤生长和进展的有效且持久的体内免疫控制。
