BioNovion/Aduro Biotech Europe, Oss, The Netherlands.
Discovery, Preclinical and Translational Medicine, Merck & Co Inc, Kenilworth, New Jersey, USA.
J Immunother Cancer. 2022 Sep;10(9). doi: 10.1136/jitc-2022-005049.
Immune checkpoint inhibitors (ICI) have radically changed cancer therapy, but most patients with cancer are unresponsive or relapse after treatment. MK-5890 is a CD27 agonist antibody intended to complement ICI therapy. CD27 is a member of the tumor necrosis factor receptor superfamily that plays a critical role in promoting responses of T cells, B cells and NK cells.
Anti-CD27 antibodies were generated and selected for agonist activity using NF-кB luciferase reporter assays. Antibodies were humanized and characterized for agonism using in vitro T-cell proliferation assays. The epitope recognized on CD27 by MK-5890 was established by X-ray crystallography. Anti-tumor activity was evaluated in a human CD27 knock-in mouse. Preclinical safety was tested in rhesus monkeys. Pharmacodynamic properties were examined in mouse, rhesus monkeys and a phase 1 dose escalation clinical study in patients with cancer.
Humanized anti-CD27 antibody MK-5890 (hIgG1) was shown to bind human CD27 on the cell surface with sub-nanomolar potency and to partially block binding to its ligand, CD70. Crystallization studies revealed that MK-5890 binds to a unique epitope in the cysteine-rich domain 1 (CRD1). MK-5890 activated CD27 expressed on 293T NF-κB luciferase reporter cells and, conditional on CD3 stimulation, in purified CD8+ T cells without the requirement of crosslinking. Functional Fc-receptor interaction was required to activate CD8+ T cells in an ex vivo tumor explant system and to induce antitumor efficacy in syngeneic murine subcutaneous tumor models. MK-5890 had monotherapy efficacy in these models and enhanced efficacy of PD-1 blockade. MK-5890 reduced in an isotype-dependent and dose-dependent manner circulating, but not tumor-infiltrating T-cell numbers in these mouse models. In rhesus monkey and human patients, reduction in circulating T cells was transient and less pronounced than in mouse. MK-5890 induced transient elevation of chemokines MCP-1, MIP-1α, and MIP-1β in the serum of mice, rhesus monkeys and patients with cancer. MK-5890 was well tolerated in rhesus monkeys and systemic exposure to MK-5890 was associated with CD27 occupancy at all doses.
MK-5890 is a novel CD27 agonistic antibody with the potential to complement the activity of PD-1 checkpoint inhibition in cancer immunotherapy and is currently undergoing clinical evaluation.
免疫检查点抑制剂(ICI)彻底改变了癌症治疗方法,但大多数癌症患者在治疗后无反应或复发。MK-5890 是一种 CD27 激动剂抗体,旨在补充 ICI 治疗。CD27 是肿瘤坏死因子受体超家族的成员,在促进 T 细胞、B 细胞和 NK 细胞的反应中发挥关键作用。
使用 NF-кB 荧光素酶报告基因检测法生成和选择抗 CD27 抗体以产生激动剂活性。使用体外 T 细胞增殖试验对抗体进行人源化和激动剂作用表征。通过 X 射线晶体学确定 MK-5890 在 CD27 上识别的表位。在人 CD27 敲入小鼠中评估抗肿瘤活性。在恒河猴中测试临床前安全性。在小鼠、恒河猴和癌症患者的 I 期剂量递增临床研究中检查药效学特性。
人源化抗 CD27 抗体 MK-5890(hIgG1)被证明以亚纳摩尔效力结合细胞表面上的人 CD27,并部分阻断与其配体 CD70 的结合。结晶研究表明,MK-5890 结合在富含半胱氨酸的结构域 1(CRD1)中的独特表位。MK-5890 激活了 293T NF-κB 荧光素酶报告细胞上表达的 CD27,并且在没有交联的情况下,在纯化的 CD8+T 细胞中,在 CD3 刺激的条件下,激活 CD27。需要功能性 Fc 受体相互作用才能在体外肿瘤外植体系统中激活 CD8+T 细胞,并在同种异体小鼠皮下肿瘤模型中诱导抗肿瘤功效。MK-5890 在这些模型中具有单药疗效,并增强了 PD-1 阻断的疗效。MK-5890 以依赖于同种型和剂量依赖性的方式减少了这些小鼠模型中循环但不浸润肿瘤的 T 细胞数量。在恒河猴和人类患者中,循环 T 细胞的减少在程度上比在小鼠中短暂且不明显。MK-5890 在小鼠、恒河猴和癌症患者的血清中诱导趋化因子 MCP-1、MIP-1α 和 MIP-1β 的短暂升高。MK-5890 在恒河猴中耐受良好,并且全身暴露于 MK-5890 与所有剂量下的 CD27 占有率相关。
MK-5890 是一种新型 CD27 激动性抗体,有可能补充癌症免疫治疗中 PD-1 检查点抑制的活性,目前正在进行临床评估。
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