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首页> 外文期刊>The Journal of Nuclear Medicine >Biodistribution and Therapeutic Efficacy of (125/131)I-, (186)Re-, (88/90)Y-, or (177)Lu-Labeled Monoclonal Antibody MN-14 to Carcinoembryonic Antigen in Mice with Small Peritoneal Metastases of Colorectal Origin.
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Biodistribution and Therapeutic Efficacy of (125/131)I-, (186)Re-, (88/90)Y-, or (177)Lu-Labeled Monoclonal Antibody MN-14 to Carcinoembryonic Antigen in Mice with Small Peritoneal Metastases of Colorectal Origin.

机译:(125/131)I-,(186)Re-,(88/90)Y-或(177)Lu标签单克隆抗体MN-14在结直肠小腹膜转移小鼠中对癌胚抗原的生物分布和治疗功效起源。

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摘要

Therapeutic efficacy in radioimmunotherapy depends, among other things, on the choice of the radionuclide. The aim of the present study was to determine the most suitable radionuclide for radioimmunotherapy with monoclonal antibody MN-14 to carcinoembryonic antigen in an experimental model of small peritoneal metastases of colorectal origin. METHODS: In nude mice with intraperitoneal LS174T tumors (diameter, 1-3 mm), the biodistributions of MN-14 labeled with (131)I ((131)I-MN-14), (186)Re-mercaptoacetyltriglycine ((186)Re-MN-14), and (88)Y-diethylenetriaminepentaacetic acid (DTPA) ((88)Y-MN-14) after intravenous and intraperitoneal administration were determined. Subsequently, the therapeutic efficacies of equally toxic activity doses of (131)I-MN-14 (9.25 MBq per mouse), (186)Re-MN-14 (9.25 MBq per mouse), (90)Y-MN-14 (3.15 MBq per mouse), and MN-14 labeled with (177)Lu-DTPA ((177)Lu-MN-14) (8.33 MBq per mouse) after intraperitoneal administration were determined. RESULTS: Each of the radioimmunoconjugates preferentially accumulated in tumor nodules, both after intravenous administration and after intraperitoneal administration. Values for clearance from blood were similar for all radioimmunoconjugates. The uptake of (88)Y-MN-14 in the liver and spleen was significantly higher than the uptake of (131)I-MN-14 or (186)Re-MN-14. Maximal uptake values (mean +/- SD) in tumors were 58 +/- 7 percentage injected dose per gram of tissue (%ID/g) for (131)I-MN-14 (24 h after administration), 83 +/- 19 %ID/g for (186)Re-MN-14 (72 h after administration), and 148 +/- 89 %ID/g for (88)Y-MN-14 (192 h after administration). Dosimetric analysis of the biodistribution data estimated that the radiation doses guided to the tumor by intraperitoneally administered (131)I-MN-14, (186)Re-MN-14, (90)Y-MN-14, and (177)Lu-MN-14 were 150, 100, 45, and 200 Gy, respectively. The median survival time of control mice, treated with unlabeled MN-14, was 42 d, whereas the median survival times of mice treated with (131)I-MN-14, (186)Re-MN-14, (90)Y-MN-14, and (177)Lu-MN-14 were 100 d (range, 58-142; P < 0.0001), 72 d (range, 46-84; P = 0.0002), 82 d (range, 46-142; P < 0.0001), and 136 d (range, 56-142; P < 0.0001), respectively. At the completion of the experiment (142 d after tumor cell inoculation), no residual disease was found in 8 of 9 long-term survivors ((131)I, n = 3; (90)Y, n = 1; and (177)Lu, n = 4). CONCLUSION: The uptake of (88)Y-MN-14 in small peritoneal LS174T xenografts was higher than the uptake of (131)I-MN-14 or (186)Re-MN-14. The present study indicates that (131)I and (177)Lu are the most suitable radionuclides for the radioimmunotherapy of small peritoneal metastases.
机译:放射免疫疗法的治疗功效尤其取决于放射性核素的选择。本研究的目的是在大肠源性小腹膜转移实验模型中,确定最合适的放射性核素,用于抗癌胚抗原的单克隆抗体MN-14进行放射免疫治疗。方法:在患有腹膜内LS174T肿瘤(直径1-3 mm)的裸鼠中,用(131)I((131)I-MN-14),(186)巯基乙酰基三甘氨酸((186测定)静脉内和腹膜内给药后)(Re-MN-14)和(88)Y-二亚乙基三胺五乙酸(DTPA)((88)Y-MN-14)。随后,以相同毒性活动剂量的(131)I-MN-14(每只小鼠9.25 MBq),(186)Re-MN-14(每只小鼠9.25 MBq),(90)Y-MN-14(确定腹膜内给药后,用(177)Lu-DTPA((177)Lu-MN-14)(每只小鼠8.33MBq)标记的MN-14(每只小鼠3.15MBq)。结果:在静脉内给药和腹膜内给药后,每种放射免疫缀合物均优先聚集在肿瘤结节中。对于所有放射免疫缀合物,从血液中清除的值均相似。肝和脾中(88)Y-MN-14的摄取显着高于(131)I-MN-14或(186)Re-MN-14的摄取。 (131)I-MN-14(给药后24小时),肿瘤的最大摄取值(平均+/- SD)为每克组织注射剂量的58 +/- 7%(%ID / g),83 + / -(186)Re-MN-14(给药后72 h)为19%ID / g,(88)Y-MN-14(给药后192 h)为148 +/- 89%ID / g。剂量分布分析的生物分布数据估计通过腹膜内施用(131)I-MN-14,(186)Re-MN-14,(90)Y-MN-14和(177)Lu引导至肿瘤的辐射剂量-MN-14分别为150、100、45和200 Gy。用未标记的MN-14处理的对照组小鼠的中位生存时间为42 d,而用(131)I-MN-14,(186)Re-MN-14,(90)Y处理的小鼠的中位生存时间-MN-14和(177)Lu-MN-14分别为100 d(范围58-142; P <0.0001),72 d(范围46-84; P = 0.0002),82 d(范围46- 142; P <0.0001)和136 d(范围56-142; P <0.0001)。在实验完成时(肿瘤细胞接种后142天),在9位长期幸存者中有8位没有发现残留疾病((131)I,n = 3;(90)Y,n = 1;和(177 Lu,n = 4)。结论:小腹膜LS174T异种移植物中(88)Y-MN-14的摄取高于(131)I-MN-14或(186)Re-MN-14的摄取。本研究表明(131)I和(177)Lu是最适合于小腹膜转移瘤放射免疫治疗的放射性核素。

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