van Gog F B, Brakenhoff R H, Snow G B, van Dongen G A
Department of Otolaryngology/Head and Neck Surgery, Free University Hospital, Amsterdam, The Netherlands.
Cancer Immunol Immunother. 1997 Apr;44(2):103-11. doi: 10.1007/s002620050362.
At our laboratory we are currently evaluating the suitability of mouse/human chimeric monoclonal antibodies (cmAb) for use in radioimmunotherapy of patients with head and neck squamous cell carcinoma (HNSCC). We have developed cmAb containing the human constant IgG1 domain and the variable domains of murine mAb (mmAb) E48 and U36 respectively. We considered the tumour-bearing nude mouse to be a well-validated model for a first testing of the targeting capabilities of these cmAb in comparison with the mmAb. Therefore, 3 microg cmAb E48 (labelled with (125)I) and 3 microg mmAb E48 (labelled with (131)I) were simultaneously injected into HNSCC-bearing nude mice and, at various assay times, mAb uptake in blood and other tissues was assessed. Remarkably, while in roughly 50% of the animals the biodistribution of the conjugates was similar, in the other animals cmAb E48 showed a much higher blood clearance than mmAb E48. This resulted in a lower tumour uptake of cmAb E48 in comparison with mmAb E48. To determine whether this phenomenon was related to mAb E48 or to the animal model, other cmAb-mmAb combinations were evaluated in the same way: cmAbs SF-25, 17-1A and U36 (all IgG1) were tested and all showed a rapid elimination in about 50% of the animals. Besides a decrease in blood concentration, an increase of cmAb levels in liver and spleen was observed within 24 h after injection. Isotype-specific enzyme-linked immunosorbent assays showed that mice that demonstrated a rapid elimination of cmAb from the blood had much lower endogenous IgGI, IgG2b and IgG3 titres than mice showing normal clearance. IgG2a levels were low in all mice. Biodistribution experiments with 3 microg chimeric 17-1A isoforms showed high blood clearance in a proportion of the mice for IgG1, IgG3 and IgG4, but not for IgG2. Increase of the cmAb dose to 100 microg resulted in a similar cmAb and mmAb biodistribution in all mice. Moreover, the biodistribution of the F(ab')2 fragment of an IgG1 cmAb was similar for all mice in contrast to that of coinjected whole IgG. On the basis of these results it can be hypothesized that, in mice with low endogenous IgG titres, cmAb with specific isotypes are rapidly removed from the blood (and ultimately from the body) by mediation of Fc-binding receptors. Apparently, in mice with high endogenous IgG titres or in mice receiving a high cmAb dose, these receptors are saturated. Furthermore, the rapid elimination of cmAb from nude mice, which may occur after injection at a low dose, is a phenomenon related to the nude mouse model.
在我们实验室,目前正在评估小鼠/人嵌合单克隆抗体(cmAb)用于头颈部鳞状细胞癌(HNSCC)患者放射免疫治疗的适用性。我们分别开发了包含人恒定IgG1结构域和鼠单克隆抗体(mmAb)E48及U36可变结构域的cmAb。与mmAb相比,我们认为荷瘤裸鼠是用于首次测试这些cmAb靶向能力的经过充分验证的模型。因此,将3μg cmAb E48(用¹²⁵I标记)和3μg mmAb E48(用¹³¹I标记)同时注射到荷HNSCC的裸鼠体内,并在不同检测时间评估血液和其他组织中抗体的摄取情况。值得注意的是,虽然在大约50%的动物中偶联物的生物分布相似,但在其他动物中,cmAb E48的血液清除率比mmAb E48高得多。这导致与mmAb E48相比,cmAb E48在肿瘤中的摄取较低。为了确定这种现象是与mAb E48有关还是与动物模型有关,以同样的方式评估了其他cmAb-mmAb组合:测试了cmAb SF-25、17-1A和U36(均为IgG1),所有这些在大约50%的动物中都显示出快速清除。除了血液浓度降低外,注射后24小时内肝脏和脾脏中cmAb水平升高。同种型特异性酶联免疫吸附测定表明,血液中cmAb快速清除的小鼠其内源性IgG1、IgG2b和IgG3滴度比清除正常的小鼠低得多。所有小鼠的IgG2a水平都很低。用3μg嵌合17-1A同种型进行的生物分布实验表明,对于IgG1、IgG3和IgG4,一部分小鼠的血液清除率很高,但IgG2并非如此。将cmAb剂量增加到100μg导致所有小鼠中cmAb和mmAb的生物分布相似。此外,与共同注射的完整IgG相比,IgG1 cmAb的F(ab')2片段在所有小鼠中的生物分布相似。基于这些结果,可以推测,在内源性IgG滴度低的小鼠中,具有特定同种型的cmAb通过Fc结合受体的介导从血液(最终从体内)快速清除。显然,在内源性IgG滴度高的小鼠或接受高剂量cmAb的小鼠中,这些受体被饱和。此外,低剂量注射后裸鼠中cmAb的快速清除是与裸鼠模型相关的现象。