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67Cu标记的完整及片段化抗结肠癌单克隆抗体MAb35的临床前评估

Preclinical evaluation of 67Cu-labeled intact and fragmented anti-colon carcinoma monoclonal antibody MAb35.

作者信息

Smith A, Alberto R, Blaeuenstein P, Novak-Hofer I, Maecke H R, Schubiger P A

机构信息

Paul Scherrer Institute, Wuerenlingen, Switzerland.

出版信息

Cancer Res. 1993 Dec 1;53(23):5727-33.

PMID:8242629
Abstract

The anti-carcinoembryonic antigen murine monoclonal antibody MAb35 and its F(ab')2 fragment were labeled with 131I or the potential therapeutic nuclide 67Cu. In vivo distribution patterns were compared in nude mice bearing human tumor xenografts by coinjection of the 131I- and 67Cu-labeled materials, thereby minimizing variations due to xenograft and host animal. The results showed that the 67Cu-labeled intact MAb35 achieved twice the percentage of injected dose/g tumor when compared to its 131I-labeled counterpart, without significant impairment of the wholebody distribution pattern. However, this effect was not evident in the case of F(ab')2, where high uptake of 67Cu was found in the kidney without any enhancement of accumulation in the target xenografts. To investigate the underlying causes of the different distribution patterns observed, iodine labeling was also performed using a more stable linkage, and the results indicated that the observed differences cannot be explained by simple deiodination of conventionally labeled preparations. We conclude that the intact form of the 67Cu-labeled antibody may be superior to the F(ab')2 fragment for use in our intended clinical studies. Our continuing work on the processing of radiometal-labeled F(ab')2 fragments, at the systemic and cellular level, will hopefully lead to a strategy to circumvent the problem of high kidney accumulation.

摘要

抗癌胚抗原鼠单克隆抗体MAb35及其F(ab')2片段用131I或潜在治疗性核素67Cu进行标记。通过共同注射131I和67Cu标记的物质,比较了荷人肿瘤异种移植裸鼠体内的分布模式,从而将异种移植和宿主动物引起的变异降至最低。结果显示,与131I标记的对应物相比,67Cu标记的完整MAb35在肿瘤中的摄取量达到注射剂量/克肿瘤的两倍,且全身分布模式无明显受损。然而,F(ab')2的情况并非如此,在肾脏中发现67Cu的高摄取,而在靶异种移植瘤中的积累没有任何增加。为了研究观察到的不同分布模式的潜在原因,还使用更稳定的连接进行了碘标记,结果表明观察到的差异不能用传统标记制剂的简单脱碘来解释。我们得出结论,67Cu标记抗体的完整形式在我们预期的临床研究中可能优于F(ab')2片段。我们在全身和细胞水平上对放射性金属标记的F(ab')2片段的处理工作仍在继续,有望找到一种策略来规避肾脏高积累的问题。

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