TRION Research GmbH, Martinsried, Germany.
J Transl Med. 2012 Nov 7;10:219. doi: 10.1186/1479-5876-10-219.
Trifunctional bispecific antibodies (trAb) are a special class of bispecific molecules recruiting and activating T cells and accessory immune cells simultaneously at the targeted tumor. The new trAb Ektomab that targets the melanoma-associated ganglioside antigen GD2 and the signaling molecule human CD3 (hCD3) on T cells demonstrated potent T-cell activation and tumor cell destruction in vitro. However, the relatively low affinity for the GD2 antigen raised the question of its therapeutic capability. To further evaluate its efficacy in vivo it was necessary to establish a mouse model.
We generated the surrogate trAb Surek, which possesses the identical anti-GD2 binding arm as Ektomab, but targets mouse CD3 (mCD3) instead of hCD3, and evaluated its chemical and functional quality as a therapeutic antibody homologue. The therapeutic and immunizing potential of Surek was investigated using B78-D14, a B16 melanoma transfected with GD2 and GD3 synthases and showing strong GD2 surface expression. The induction of tumor-associated and autoreactive antibodies was evaluated.
Despite its low affinity of approximately 10(7) M(-1) for GD2, Surek exerted efficient tumor cell destruction in vitro at an EC(50) of 70 ng/ml [0.47 nM]. Furthermore, Surek showed strong therapeutic efficacy in a dose-dependent manner and is superior to the parental GD2 mono-specific antibody, while the use of a control trAb with irrelevant target specificity had no effect. The therapeutic activity of Surek was strictly dependent on CD4(+) and CD8(+) T cells, and cured mice developed a long-term memory response against a second challenge even with GD2-negative B16 melanoma cells. Moreover, tumor protection was associated with humoral immune responses dominated by IgG2a and IgG3 tumor-reactive antibodies indicating a Th1-biased immune response. Autoreactive antibodies against the GD2 target antigen were not induced.
Our data suggest that Surek revealed strong tumor elimination and anti-tumor immunization capabilities. The results warrant further clinical development of the human therapeutic equivalent antibody Ektomab.
三功能双特异性抗体(trAb)是一类特殊的双特异性分子,能够同时招募和激活靶向肿瘤的 T 细胞和辅助免疫细胞。新型 trAb Ektomab 靶向黑色素瘤相关神经节苷脂抗原 GD2 和 T 细胞上的信号分子人 CD3(hCD3),在体外显示出强大的 T 细胞激活和肿瘤细胞杀伤能力。然而,其对 GD2 抗原的亲和力相对较低,引发了对其治疗能力的质疑。为了进一步评估其体内疗效,有必要建立一个小鼠模型。
我们生成了替代 trAb Surek,它具有与 Ektomab 相同的抗 GD2 结合臂,但靶向小鼠 CD3(mCD3)而不是 hCD3,并评估了其作为治疗性抗体同源物的化学和功能质量。使用 B78-D14,即转染 GD2 和 GD3 合成酶的 B16 黑色素瘤细胞系,研究了 Surek 的治疗和免疫潜力,该细胞系表现出强烈的 GD2 表面表达。评估了肿瘤相关和自身抗体的诱导。
尽管其对 GD2 的亲和力约为 10(7) M(-1),但 Surek 在 EC(50)为 70ng/ml[0.47nM]时在体外仍能有效杀伤肿瘤细胞。此外,Surek 以剂量依赖性方式表现出强大的治疗效果,优于亲本 GD2 单特异性抗体,而使用具有无关靶特异性的对照 trAb 则没有效果。Surek 的治疗活性严格依赖于 CD4(+)和 CD8(+)T 细胞,治愈的小鼠甚至在使用 GD2 阴性 B16 黑色素瘤细胞时,对第二次挑战产生了长期记忆反应。此外,肿瘤保护与以 IgG2a 和 IgG3 肿瘤反应性抗体为主的体液免疫反应有关,表明存在 Th1 偏向的免疫反应。未诱导针对 GD2 靶抗原的自身抗体。
我们的数据表明,Surek 显示出强大的肿瘤消除和抗肿瘤免疫能力。结果证明进一步开发人类治疗等效抗体 Ektomab 是合理的。
Zotero 插件
