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裸鼠胫骨内细胞接种建立的人肿瘤模型的有效性和实用性。

Validity and usefulness of human tumor models established by intratibial cell inoculation in nude rats.

作者信息

Kjønniksen I, Winderen M, Bruland O, Fodstad O

机构信息

Department of Tumor Biology, Norwegian Radium Hospital, Oslo.

出版信息

Cancer Res. 1994 Apr 1;54(7):1715-9.

PMID:8137286
Abstract

Intratibial injection in nude rats of 1 x 10(6) OHS, MHMX, and LOX human tumor cells resulted in each case in progressively growing bone tumors. When the diameter of the affected leg had increased by 2-3 mm, the animals were examined for uptake of 99mTc-methylenediphosphonate. The OHS osteosarcoma tumors caused sclerotic lesions with high and uniform isotope uptake, and the MHMX unclassified sarcoma showed a mixed pattern with both sclerotic and lytic areas, whereas the LOX melanoma caused lytic bone lesions with low uptake of the radionuclide. These findings were compared with the results of analogous investigations previously performed in the patients from whom the tumor lines originated. Striking similarities in both the morphology and the scintigraphic images were observed between corresponding tumors in rats and humans, with results supporting the clinical relevance of the model systems. When the LOX model was used for therapy experiments, doxorubicin had no effect on the growth of the tibial tumors, which in the control group appeared after a latency of 13.5 days. The alkylating agent mitozolomide increased the median tumor-free latency to 47 days in 7 rats, and 5 animals did not develop tumors within the observation period of 60 days. Doxorubicin was ineffective also against the OHS tumor, whereas ifosfamide and the radionuclide 89Sr-chloride showed significant antitumor activity. The disease-free latency increased from 20 days, in the control animals, to 45 and 28.5 days, respectively, in the 2 treated groups, in which 2 of 7 and 2 of 10 rats were without tumors at 60 days. The data demonstrate that the tibial models discriminated between the action of the different therapeutic agents, and suggest that they may be useful in selecting compounds with clinical activity against skeletal tumors.

摘要

将1×10⁶个OHS、MHMX和LOX人肿瘤细胞注射到裸鼠胫骨内,每种情况均导致骨肿瘤逐渐生长。当患侧腿的直径增加2 - 3毫米时,检查动物对99mTc - 亚甲基二膦酸盐的摄取情况。OHS骨肉瘤肿瘤导致硬化性病变,同位素摄取高且均匀,而MHMX未分类肉瘤呈现硬化和溶解区域的混合模式,而LOX黑色素瘤导致溶骨性骨病变,放射性核素摄取低。这些发现与先前在肿瘤系起源患者中进行的类似研究结果进行了比较。在大鼠和人类的相应肿瘤之间,在形态学和闪烁图像上均观察到显著相似性,结果支持了模型系统的临床相关性。当将LOX模型用于治疗实验时,阿霉素对胫骨肿瘤的生长没有影响,对照组在13.5天的潜伏期后出现肿瘤。烷化剂米托唑胺使7只大鼠的无肿瘤中位潜伏期增加到47天,5只动物在60天的观察期内未发生肿瘤。阿霉素对OHS肿瘤也无效,而异环磷酰胺和放射性核素89Sr - 氯化物显示出显著的抗肿瘤活性。无病潜伏期从对照动物的20天分别增加到两个治疗组的45天和28.5天,在这两个治疗组中,7只大鼠中有2只和10只大鼠中有2只在60天时无肿瘤。数据表明胫骨模型能够区分不同治疗药物的作用,并表明它们可能有助于选择对骨骼肿瘤具有临床活性的化合物。

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