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去岩藻糖基化抗CCR4单克隆抗体在NOD/Shi-scid、IL-2Rγ(缺失)小鼠体内对由自体人类免疫细胞介导的原发性成人T细胞白血病/淋巴瘤(ATLL)细胞发挥强大的抗体依赖的细胞介导的细胞毒性作用(ADCC)。

Defucosylated anti-CCR4 monoclonal antibody exerts potent ADCC against primary ATLL cells mediated by autologous human immune cells in NOD/Shi-scid, IL-2R gamma(null) mice in vivo.

作者信息

Ito Asahi, Ishida Takashi, Utsunomiya Atae, Sato Fumihiko, Mori Fumiko, Yano Hiroki, Inagaki Atsushi, Suzuki Susumu, Takino Hisashi, Ri Masaki, Kusumoto Shigeru, Komatsu Hirokazu, Iida Shinsuke, Inagaki Hiroshi, Ueda Ryuzo

机构信息

Department of Medical Oncology and Immunology, Nagoya City University Graduate School of Medical Sciences, Nagoya, Aichi 467-8601, Japan.

出版信息

J Immunol. 2009 Oct 1;183(7):4782-91. doi: 10.4049/jimmunol.0900699. Epub 2009 Sep 11.

DOI:10.4049/jimmunol.0900699
PMID:19748990
Abstract

There is a lack of suitable small animal models to evaluate human Ab-dependent cellular cytotoxicity (ADCC) in vivo, because of the species incompatibility between humans and animals or due to nonspecific allogeneic immune reactions. To overcome these problems, we established a human tumor-bearing mouse model, using NOD/Shi-scid, IL-2Rgamma(null) (NOG) mice as recipients, in which autologous human immune cells are engrafted and mediate ADCC but in which endogenous murine cells are unable to mediate ADCC. In the present study, we used NOG mice bearing primary adult T cell leukemia/lymphoma (ATLL) cells and a therapeutic chimeric anti-CCR4 mAb, the Fc region of which is defucosylated to enhance ADCC. We report significant antitumor activity in vivo associated with robust ADCC mediated by autologous effector cells from the same patients. The present study is the first to report a mouse model in which a potent antitumor effect of the therapeutic mAb against primary tumor cells is mediated by autologous human immune cells. Human autologous ADCC in mice in vivo was confirmed by the depletion of human immune cells before ATLL PBMC inoculation. In addition, NOG mice bearing primary ATLL cells presented features identical with patients with ATLL. In conclusion, this approach makes it possible to model the human immune system active in Ab-based immunotherapy in vivo, and thus to perform more appropriate preclinical evaluations of novel therapeutic mAb. Furthermore, the potent ADCC mediated by defucosylated anti-CCR4 mAb, observed here in vivo in humanized mice, will be exploited in clinical trials in the near future.

摘要

由于人和动物之间的物种不相容性或由于非特异性同种异体免疫反应,缺乏合适的小动物模型来在体内评估人抗体依赖性细胞毒性(ADCC)。为了克服这些问题,我们建立了一种荷人肿瘤小鼠模型,使用NOD/Shi-scid、IL-2Rγ(null)(NOG)小鼠作为受体,在该模型中植入自体人免疫细胞并介导ADCC,但内源性鼠细胞无法介导ADCC。在本研究中,我们使用了携带原发性成人T细胞白血病/淋巴瘤(ATLL)细胞的NOG小鼠和一种治疗性嵌合抗CCR4单克隆抗体(mAb),其Fc区域去岩藻糖基化以增强ADCC。我们报告了与来自同一患者的自体效应细胞介导的强大ADCC相关的显著体内抗肿瘤活性。本研究首次报道了一种小鼠模型,其中治疗性单克隆抗体对原发性肿瘤细胞的有效抗肿瘤作用由自体人免疫细胞介导。在接种ATLL外周血单核细胞(PBMC)之前通过耗尽人免疫细胞证实了小鼠体内人自体ADCC。此外,携带原发性ATLL细胞的NOG小鼠呈现出与ATLL患者相同的特征。总之,这种方法使得在体内模拟基于抗体的免疫治疗中活跃的人免疫系统成为可能,从而能够对新型治疗性单克隆抗体进行更合适的临床前评估。此外,在人源化小鼠体内观察到的去岩藻糖基化抗CCR4单克隆抗体介导的强大ADCC将在不久的将来用于临床试验。

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