Anti-angiogenic therapy and radioimmunotherapy in colon cancer xenografts

被引:0
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作者
Seigo Kinuya
Atsuhiro Kawashima
Kunihiko Yokoyama
Miho Kudo
Yoshihito Kasahara
Naoto Watanabe
Noriyuki Shuke
Hisashi Bunko
Takatoshi Michigishi
Norihisa Tonami
机构
[1] Department of Nuclear Medicine,
[2] Kanazawa University School of Medicine,undefined
[3] 13-1 Takaramachi,undefined
[4] Kanazawa,undefined
[5] Ishikawa,undefined
[6] 920-8640 Japan,undefined
[7] Department of Pathology (I),undefined
[8] Kanazawa University School of Medicine,undefined
[9] Kanazawa,undefined
[10] Ishikawa,undefined
[11] Department of Pediatrics,undefined
[12] Kanazawa University School of Medicine,undefined
[13] Kanazawa,undefined
[14] Ishikawa,undefined
[15] Department of Radiology,undefined
[16] Toyama Medical and Pharmaceutical University,undefined
[17] Toyama,undefined
[18] Department of Radiology,undefined
[19] Asahikawa Medical College,undefined
[20] Asahikawa,undefined
[21] Medical Informatics,undefined
[22] Kanazawa University Hospital,undefined
[23] Kanazawa,undefined
来源
关键词
Radioimmunotherapy 2-Methoxyestradiol Anti-angiogenesis;
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摘要
Angiogenesis is critical to the growth and metastatic process of malignant tumors. An endogenous estrogen metabolite, 2-methoxyestradiol (2-ME), displays anti-angiogenic and anti-tumorigenic effects. The purpose of this investigation was to determine whether exogenously administered 2-ME would enhance the efficacy of radioimmunotherapy (RIT). Experimental RIT with 4.63 MBq of 131I-A7, an IgG1 anti-colorectal monoclonal antibody, was conducted in mice xenografted with LS180 human colon cancer cells. 2-ME suspended in 0.5% carboxymethylcellulose was administered daily at a dose of 75 mg/kg per day. 2-ME administration suppressed tumor growth and improved the efficacy of RIT in comparison to RIT alone. Tumor volumes on day 13, expressed as a ratio relative to the initial volume, were 12.7±2.95 in the nontreated control, 4.73±0.89 with 2-ME, 3.05±0.37 with RIT and 0.97±0.20 with RIT+2-ME. Immunohistochemistry of tumor sections stained with an antibody against factor VIII demonstrated a decrease in microvessel number within tumors treated with 2-ME (7.9±0.8/200× field) as compared with that in control tumors (29.9±2.5). Cell proliferation assay at increasing concentrations of 2-ME showed direct cytotoxicity of 2-ME in vitro at 5 µM and greater. In conclusion, 2-ME enhanced the efficacy of RIT with 131I-A7 via inhibition of angiogenesis within the xenografts. The direct cytotoxicity of 2-ME appears to have contributed to this improvement. Anti-angiogenic therapy may prolong the dormancy of microscopic metastases while RIT may exterminate this population of cells. Therefore, the combined treatment may improve the therapeutic outcome of patients with disseminated cancer.
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页码:1306 / 1312
页数:6
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