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放射性标记抗体在裸鼠实验性肝转移模型中的瘤内分布及放射免疫治疗

Intratumoral distribution of radiolabeled antibody and radioimmunotherapy in experimental liver metastases model of nude mouse.

作者信息

Sato N, Saga T, Sakahara H, Yao Z, Nakamoto Y, Zhang M, Kuroki M, Matsuoka Y, Iida Y, Konishi J

机构信息

Department of Nuclear Medicine and Diagnostic Imaging, Kyoto University, Sakyo, Japan.

出版信息

J Nucl Med. 1999 Apr;40(4):685-92.

Abstract

UNLABELLED

The biodistribution and intratumoral distribution of radiolabeled anticarcinoembryonic antigen (CEA) monoclonal antibody in experimental liver metastases and the therapeutic effect of 131I-labeled anti-CEA antibody on the metastases were studied.

METHODS

Three weeks after an intrasplenic injection of human colon cancer cells, mice received an intravenous injection of 125I- or 111In-labeled anti-CEA antibody F33-104. The biodistribution and tumor penetration of radiolabeled antibody were examined by using quantitative autoradiography. To evaluate the therapeutic effect, 5.55, 9.25 or 11.1 MBq (150, 250 or 300 microCi) 131I-labeled F33-104 were injected into groups of mice that had micrometastases smaller than 1 mm. Control groups were injected with phosphate-buffered saline or 131I-labeled control antibody. Mice were killed 3 wk later to determine the size of liver metastases.

RESULTS

1251-labeled F33-104 showed a high accumulation in the liver metastases (percentage of injected dose per gram of metastases [%ID/g] >24%, metastasis-to-liver ratio >9.8, metastasis-to-blood ratio >2.1); however, its accumulation was heterogeneous or peripheral in the nodules more than 1 mm in diameter. When the antibody dose was increased, antibody penetration was improved, but tumor uptake of radioactivity and specificity ratios decreased. In mice with large metastases, radioactivity in the normal tissue was lower than that in mice with small metastases, resulting in higher metastasis-to-background ratios. 111In-labeled antibody showed even higher tumor uptake than 125I-labeled antibody (>51 %ID/g). Metastases formation was suppressed in a dose-dependent manner by 131I-labeled F33-104 injection (5 of 8 mice had no macroscopic tumor after an injection of 5.55 MBq (150 microCi), and all mice had no visible metastasis after an injection of 9.25 or 11.1 MBq [250 or 300 microCi]), whereas tumor progression was seen in the control groups.

CONCLUSION

Liver metastases had easy accessibility to the antibody. Micrometastases of less than 0.5 mm in diameter showed homogeneous intratumoral distribution of injected antibody and were successfully treated with 131I-labeled antibody. Very high uptake and satisfactory metastasis-to-liver ratios with 111In-labeled antibody suggest that the use of a radiometal with high beta-energy, such as 90Y or 188Re, is preferable for the successful radioimmunotherapy of metastases larger than 1 mm.

摘要

未标记

研究了放射性标记的抗癌胚抗原(CEA)单克隆抗体在实验性肝转移瘤中的生物分布和瘤内分布,以及131I标记的抗CEA抗体对转移瘤的治疗效果。

方法

在脾内注射人结肠癌细胞3周后,小鼠静脉注射125I或111In标记的抗CEA抗体F33-104。通过定量放射自显影检查放射性标记抗体的生物分布和肿瘤穿透情况。为评估治疗效果,将5.55、9.25或11.1 MBq(150、250或300微居里)的131I标记的F33-104注射到有小于1mm微小转移灶的小鼠组中。对照组注射磷酸盐缓冲盐水或131I标记的对照抗体。3周后处死小鼠以确定肝转移灶的大小。

结果

125I标记的F33-104在肝转移瘤中显示出高蓄积(每克转移灶注射剂量的百分比[%ID/g]>24%,转移灶与肝脏的比值>9.8,转移灶与血液的比值>2.1);然而,其在直径大于1mm的结节中的蓄积是不均匀的或位于周边。当抗体剂量增加时,抗体穿透性得到改善,但肿瘤对放射性的摄取和特异性比值降低。在有大转移灶的小鼠中,正常组织中的放射性低于有小转移灶的小鼠,导致转移灶与背景的比值更高。111In标记的抗体显示出比125I标记的抗体更高的肿瘤摄取(>51%ID/g)。131I标记的F33-104注射以剂量依赖的方式抑制转移灶形成(注射5.55 MBq(150微居里)后,8只小鼠中有5只无肉眼可见肿瘤,注射9.25或11.1 MBq[250或3C0微居里]后,所有小鼠均无可见转移灶),而对照组中可见肿瘤进展。

结论

肝转移瘤易于摄取抗体。直径小于0.5mm的微小转移灶显示注射的抗体在瘤内分布均匀,并用131I标记的抗体成功治疗。111In标记的抗体具有非常高的摄取和令人满意的转移灶与肝脏比值,这表明使用具有高β能量的放射性金属,如90Y或188Re,对于成功地对大于1mm的转移瘤进行放射免疫治疗是更可取的。

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