使用213Bi偶联单克隆抗体的分次局部低剂量放射免疫疗法可提高弥漫型胃癌小鼠模型的生存率。

Fractionated locoregional low-dose radioimmunotherapy improves survival in a mouse model of diffuse-type gastric cancer using a 213Bi-conjugated monoclonal antibody.

作者信息

Bloechl Stefanie, Beck Roswitha, Seidl Christof, Morgenstern Alfred, Schwaiger Markus, Senekowitsch-Schmidtke Reingard

机构信息

Department of Nuclear Medicine, Technische Universität München, Germany.

出版信息

Clin Cancer Res. 2005 Oct 1;11(19 Pt 2):7070s-7074s. doi: 10.1158/1078-0432.CCR-1004-0017.

DOI:10.1158/1078-0432.CCR-1004-0017

PMID:16203804

Abstract

PURPOSE

Locoregional radioimmunotherapy of i.p. tumor cell dissemination of diffuse-type gastric cancer using the alpha-emitter 213Bi displayed good therapeutic results after a single application depending on the time interval between tumor cell inoculation and injection of the 213Bi-immunoconjugate. The aim of the present study was to compare single versus double i.p. injection of a tumor-specific antibody (d9MAb) conjugated with low activities of 213Bi in terms of therapeutic efficacy and toxicity.

EXPERIMENTAL DESIGN

Nude mice were inoculated i.p. with 1 x 10(7) human gastric cancer cells (HSC45-M2) expressing tumor-specific mutant d9-E-cadherin (d9-E-cad). After tumor cell inoculation, the mice were injected i.p. with a single injection at day 1 or 8, or double injections at days 1 and 8 or days 8 and 15 with 0.37, 0.74, or 1.48 MBq 213Bi-d9MAb. Therapeutic efficacy was determined by median survival, and toxicity was evaluated by leukocyte and platelet counts. The development of i.p. carcinomatosis was monitored by carcinoembryonic antigen concentrations in the serum of the mice.

RESULTS

The median survival of treated animals increased, depending on the time interval (days) between tumor cell inoculation and therapy, and the injected activity, from 22 days of untreated mice to 48 days (0.37 MBq, 1 day), 84 days (0.37 MBq, 1 and 8 days), 37 days (0.37 MBq, 8 days), 46 days (0.37 MBq, 8 and 15 days), 42 days (0.74 MBq, 8 days), 78 days (0.74 MBq, 8 and 15 days), and 44 days (1.48 MBq, 8 days). The injected activities did not reduce leukocyte and platelet counts. Carcinoembryonic antigen, which was not detectable in the serum of tumor-free mice, increased after tumor cell inoculation and tumor proliferation and decreased after each therapeutic application of 213Bi-d9MAb.

CONCLUSIONS

Double application of only 0.37 MBq of 213Bi-d9MAb at days 1 and 8 after tumor cell inoculation significantly prolonged median survival in nude mice suffering from i.p. tumor cell dissemination compared with a single injection. Even in an advanced stage of the disease, double injection of 0.74 MBq at days 8 and 15 was superior to a single injection of 1.48 MBq at day 8 without any sign of toxicity.

摘要

目的

使用α发射体213Bi对弥漫型胃癌腹腔内肿瘤细胞播散进行局部区域放射免疫治疗，单次应用后根据肿瘤细胞接种与213Bi免疫缀合物注射之间的时间间隔显示出良好的治疗效果。本研究的目的是比较单次与两次腹腔内注射与低活度213Bi偶联的肿瘤特异性抗体（d9MAb）在治疗效果和毒性方面的差异。

实验设计

将表达肿瘤特异性突变d9-E-钙黏蛋白（d9-E-cad）的1×10⁷人胃癌细胞（HSC45-M2）腹腔接种于裸鼠。肿瘤细胞接种后，小鼠于第1天或第8天单次腹腔注射，或于第1天和第8天或第8天和第15天两次腹腔注射0.37、0.74或1.48 MBq的213Bi-d9MAb。通过中位生存期确定治疗效果，通过白细胞和血小板计数评估毒性。通过小鼠血清中癌胚抗原浓度监测腹腔内癌的发展。

结果

治疗动物的中位生存期根据肿瘤细胞接种与治疗之间的时间间隔（天）和注射活度而增加，从未治疗小鼠的22天增加到48天（0.37 MBq，第1天）、84天（0.37 MBq，第1天和第8天）、37天（0.37 MBq，第8天）、46天（0.37 MBq，第8天和第15天）、42天（0.74 MBq，第8天）、78天（0.74 MBq，第8天和第15天）和44天（1.48 MBq，第8天）。注射活度未降低白细胞和血小板计数。在无肿瘤小鼠血清中不可检测的癌胚抗原，在肿瘤细胞接种和肿瘤增殖后增加，在每次213Bi-d9MAb治疗应用后降低。