In vivo properties of three human HER2/neu-expressing murine cell lines in immunocompetent mice.

Laboratory animal science Pub Date : 1999-04-01
M L Penichet, P M Challita, S U Shin, S L Sampogna, J D Rosenblatt, S L Morrison
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Abstract

Background and purpose: Expression of the HER2/neu proto-oncogene, a receptor-like transmembrane protein expressed at low levels on some normal cells, is markedly increased in a subset of human breast, colon, lung, and ovarian cancers. A humanized HER2/neu antibody has been tested as a therapeutic agent in several clinical trials, with promising results. We have developed a family of anti-HER2/neu fusion proteins. To evaluate the immunologic efficacy of these proteins, it is critical that tumors expressing the target antigen can grow in immunologically intact mice.

Method: To produce murine tumors expressing human HER2/neu on the surface, CT26, MC38, and EL4 murine cell lines were transduced by use of a retroviral construct containing the cDNA encoding the human HER2/neu gene.

Results: Histologic features and kinetics of tumor growth in subcutaneous space of the human HER2/neu-expressing cells were similar to those of the respective parental cell lines. Intravenous inoculation with these cells induced disseminated malignant disease. Flow cytometric and immmunohistochemical analyses of freshly isolated tumors revealed in vivo expression of human HER2/neu. Secretion of antigen was not detected by use of an ELISA.

Conclusion: Although an antibody response against the human HER2/neu antigen was observed, this response does not affect the growth rate of the HER2/neu-expressing cells. These murine models may be useful tools for evaluation of anti-cancer therapeutic approaches that target human HER2/neu.

三种表达人HER2/ new的小鼠细胞系在免疫功能小鼠体内的特性。
背景和目的:HER2/neu原癌基因是一种受体样跨膜蛋白,在一些正常细胞中低水平表达,在人类乳腺癌、结肠癌、肺癌和卵巢癌的一个亚群中显著增加。一种人源化的HER2/neu抗体已经在一些临床试验中作为治疗药物进行了测试,结果很有希望。我们已经开发了一个抗her2 /neu融合蛋白家族。为了评估这些蛋白的免疫功效,表达目标抗原的肿瘤能否在免疫完好的小鼠体内生长至关重要。方法:利用含有编码人HER2/neu基因cDNA的逆转录病毒构建体,对CT26、MC38和EL4小鼠细胞系进行转导,制备表面表达人HER2/neu的小鼠肿瘤。结果:人HER2/ new表达细胞的组织学特征和肿瘤在皮下间隙生长的动力学与各自亲本细胞系相似。静脉注射这些细胞诱导播散性恶性疾病。流式细胞术和免疫组织化学分析显示,新分离的肿瘤在体内表达人HER2/neu。ELISA法未检测到抗原的分泌。结论:虽然观察到针对人HER2/neu抗原的抗体反应,但这种反应不影响HER2/neu表达细胞的生长速度。这些小鼠模型可能是评估针对人类HER2/neu的抗癌治疗方法的有用工具。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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