提高肿瘤的放射免疫靶向性:预载无标记L6单克隆抗体对大鼠体内125I-L6生物分布的影响

M Garkavij, J Tennvall, S E Strand, K Norrgren, R Nilsson, H O Sjögren
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引用次数: 0

摘要

在恶性肿瘤的放射免疫治疗中,与正常组织相比,单克隆抗体(MoAb)在肿瘤中的摄取通常较低。提出了几种提高肿瘤与正常组织(T/N)比率的方法。在这项研究中,我们研究了不同量的125i -L6-生物素MoAb与未标记L6 MoAb的预负荷相结合的生物分布。在给裸大鼠注射10微克、50微克或250微克抗胰腺癌摩押125I-L6前24小时注射50微克或250微克未标记的L6。注射放射性标记的MoAb后24小时进行解剖。在正常组织中,250微克125I-L6在预负荷50微克未标记的L6之前,最大程度地增强肿瘤摄取,同时降低摄取。与相应的对照组相比,骨髓、肝脏、肺和肾脏的平均T/N比分别提高了2.9倍、3.4倍、3.7倍和2.3倍。本研究表明,预注射最佳量的未标记L6 MoAb可增加肿瘤对125I-L6的摄取,并提高T/N比。基于目前的数据,在未来的免疫偶联物临床研究中,应考虑使用未标记的MoAb预载,以提高肿瘤的放射免疫靶向性。必须滴定适量的预负荷,从而避免未标记的MoAb可能的肿瘤抗原饱和,同时减少随后在正常组织中注射放射性标记的MoAb的摄取。
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Improving radioimmunotargeting of tumors: the impact of preloading unlabeled L6 monoclonal antibody on the biodistribution of 125I-L6 in rats.

In the radioimmunotherapy of malignancies the uptake of monoclonal antibodies (MoAb) is commonly low in tumors compared with normal tissue. Several methods have been suggested to increase the tumor-to-normal tissue (T/N) ratio. In this study we have investigated the biodistribution of different amounts of 125I-L6-biotin MoAb in combination with a preload of unlabeled L6 MoAb. Nude rats were injected with 50 micrograms or 250 micrograms of unlabeled L6 24 hours prior to the injection of 10 micrograms, 50 micrograms or 250 micrograms of 125I-L6, antipancarcinoma MoAb. Dissections were performed 24 hours after the injection of radiolabeled MoAb. The maximal enhancement of tumor uptake with simultaneously decreased uptake in normal tissues was with 250 micrograms of 125I-L6 preceded by a preload of 50 micrograms unlabeled L6. Mean T/N ratios were improved by a factor of 2.9 for bone marrow, 3.4 for liver, 3.7 for lungs and 2.3 for kidneys as compared with the corresponding controls. This study demonstrated that preinjection of optimal amounts of unlabeled L6 MoAb may increase the uptake of 125I-L6 by tumor and improve the T/N ratios. Based on present data, preloading with unlabeled MoAb should be considered in future clinical studies with immunoconjugates to improve the radioimmunotargeting of tumors. It is essential to titrate an appropriate amount of the preload, thus avoiding possible tumor antigen saturation of unlabeled MoAbs but simultaneously decreasing the uptake of subsequently injected radiolabeled MoAb in normal tissues.

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