Gerretsen M, Schrijvers A H, van Walsum M, Braakhuis B J, Quak J J, Meijer C J, Snow G B, van Dongen G A
Department of Otolaryngology/Head and Neck Surgery, Free University Hospital, Amsterdam, The Netherlands.
Br J Cancer. 1992 Sep;66(3):496-502. doi: 10.1038/bjc.1992.302.
Monoclonal antibody (MAb) E48 reacts with a 22 kD antigen exclusively expressed in squamous and transitional epithelia and their neoplastic counterparts. Radiolabelled with 99mTc, MAb E48 is capable of targeting metastatic and recurrent disease in patients with head and neck cancer. In this study, the capacity of 131I-labelled MAb E48 to eradicate xenografts of human squamous cell carcinoma of the head and neck (HNSCC) in nude mice was examined. Experimental groups received a single i.v. bolus injection of 400 microCi MAb E48 IgG (number of mice (n = 6, number of tumours (t) = 9) or 800 microCi MAb E48 IgG (n) = 5,t = 7), whereas control groups received either diluent (n = 3,t = 5), unlabelled MAb E48 IgG (n = 4,t = 5) or 800 microCi 131I-labelled isotype-matched control MAb (n = 6,t = 9). A 4.1-fold increase in the median tumour volume doubling time and regression of two out of ten tumours (20%) was observed in mice treated with 400 microCi. In mice treated with 800 microCi. In mice treated with 800 microCi, two out of seven tumours (29%) showed complete remission without regrowth during follow-up (greater than 3 months). Median tumour volume doubling time in the remaining five tumours was increased 7.8-fold. No antitumour effects were observed in mice injected with diluent, unlabelled MAb E48 or 131I-labelled control MAb. In the same xenograft model, chemotherapy with doxorubicin, 5-fluorouracil, cisplatin, bleomycin, methotrexate or 2',2'-difluorodeoxycytidine yielded a less profound effect on tumour volume doubling time. Increases in tumour volume doubling time with these chemotherapeutic agents were 4, 2.2, 2.1, 1.7, 0, and 2.6 respectively. Moreover, no cures were observed with any of these chemotherapeutic agents. From the tissue distribution of 800 microCi MAb E48, the absorbed cumulative radiation doses of tumour and various organs were calculated using the trapezoid integration method for the area under the curve. To tumour xenografts, 12,170 cGy was delivered, blood received 2,984 cGy, whereas in every other tissue the accumulated dose was less than 6% of the dose delivered to tumour. These data, describing the first radiolabelled MAb with therapeutic efficacy against HNSCC, suggest radioimmunotherapy with MAb E48 to be a potential therapeutic modality for the treatment of head and neck cancer.
单克隆抗体(MAb)E48与一种仅在鳞状上皮和移行上皮及其肿瘤对应物中表达的22kD抗原发生反应。用99mTc进行放射性标记后,MAb E48能够靶向头颈部癌患者的转移性和复发性疾病。在本研究中,检测了131I标记的MAb E48根除裸鼠头颈部人鳞状细胞癌(HNSCC)异种移植物的能力。实验组接受单次静脉推注400微居里的MAb E48 IgG(小鼠数量(n = 6),肿瘤数量(t) = 9)或800微居里的MAb E48 IgG(n = 5,t = 7),而对照组接受稀释剂(n = 3,t = 5)、未标记的MAb E48 IgG(n = 4,t = 5)或800微居里的131I标记的同型匹配对照单克隆抗体(n = 6,t = 9)。在用400微居里治疗的小鼠中,观察到肿瘤体积中位倍增时间增加了4.1倍,并且十个肿瘤中有两个(20%)出现消退。在用800微居里治疗的小鼠中,七个肿瘤中有两个(29%)在随访期间(超过3个月)显示完全缓解且无复发。其余五个肿瘤的肿瘤体积中位倍增时间增加了7.8倍。在注射稀释剂、未标记的MAb E48或131I标记的对照单克隆抗体的小鼠中未观察到抗肿瘤作用。在相同的异种移植模型中,用阿霉素、5-氟尿嘧啶、顺铂、博来霉素、甲氨蝶呤或2',2'-二氟脱氧胞苷进行化疗对肿瘤体积倍增时间的影响较小。这些化疗药物使肿瘤体积倍增时间增加的倍数分别为4倍、2.2倍、2.1倍、1.7倍、0倍和2.6倍。此外,使用这些化疗药物均未观察到治愈情况。根据800微居里MAb E48的组织分布,采用梯形积分法计算曲线下面积,得出肿瘤和各个器官的吸收累积辐射剂量。对于肿瘤异种移植物,给予了12,170 cGy,血液接受了2,984 cGy,而在其他每个组织中,累积剂量均小于给予肿瘤剂量的6%。这些数据描述了第一种对HNSCC具有治疗效果的放射性标记单克隆抗体,表明用MAb E48进行放射免疫治疗可能是治疗头颈部癌的一种潜在治疗方式。