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通过股内接种肿瘤细胞建立的一种新的骨肉瘤实验大鼠模型,可用于生物学和治疗研究。

A new experimental rat model of osteosarcoma established by intrafemoral tumor cell inoculation, useful for biology and therapy investigations.

作者信息

Cherrier B, Gouin F, Heymann M-F, Thiéry J P, Rédini F, Heymann D, Duteille F

机构信息

Physiopathologie de la Résorption Osseuse et Thérapie des Tumeurs Osseuses Primitives, Faculté de Médecine, Université de Nantes EA 3822, INSERM ERI 7, Nantes, France.

出版信息

Tumour Biol. 2005 May-Jun;26(3):121-30. doi: 10.1159/000086483. Epub 2005 Jun 17.

DOI:10.1159/000086483
PMID:15970646
Abstract

Satisfactory experimental models for preclinical cancer studies must follow several criteria: (1) reproducibility of the method used to induce the tumor and (2) clinical, pathological and kinetic similarity with the corresponding human tumors. We developed a model of osteosarcoma locally induced by the intrafemoral injection of osteosarcoma (OSR) cells in Sprague-Dawley rats. This method yields nearly 80% of bone tumors at the injection site. These tumors double their volume fairly slowly (in approximately 20 days) and lung metastases occur in 96% of the animals. The OSR cell-induced tumor is characterized by a direct production of mineralized matrix by the tumor cells themselves, as revealed by histochemical analysis. The microarchitectural parameters which were quantified by a microscanner show an increased trabecular bone volume (+238%) when OSR cells were injected in the femur, as compared to controls injected with vehicle. Osteoblastic markers such as alkaline phosphatase, osteopontin, osteocalcin and bone sialoprotein were expressed by the tumor in vivo, whereas the initially injected OSR cells did not express some of these markers, suggesting that OSR cells reacquired an osteoblastic phenotype in a favorable environment. The clinical, radiological and histological data show that this model shares high similarities with the osteocondensing forms of osteosarcoma in humans.

摘要

用于临床前癌症研究的令人满意的实验模型必须符合几个标准

(1)诱导肿瘤所用方法的可重复性,以及(2)与相应人类肿瘤在临床、病理和动力学方面的相似性。我们通过在Sprague-Dawley大鼠股骨内注射骨肉瘤(OSR)细胞,建立了一种局部诱导骨肉瘤的模型。这种方法在注射部位产生近80%的骨肿瘤。这些肿瘤体积增长相当缓慢(约20天翻倍),96%的动物会发生肺转移。组织化学分析显示,OSR细胞诱导的肿瘤的特征是肿瘤细胞自身直接产生矿化基质。与注射赋形剂的对照组相比,通过微扫描仪量化的微观结构参数显示,当在股骨中注射OSR细胞时,小梁骨体积增加(+238%)。肿瘤在体内表达成骨细胞标志物,如碱性磷酸酶、骨桥蛋白、骨钙素和骨唾液蛋白,而最初注射的OSR细胞不表达其中一些标志物,这表明OSR细胞在有利环境中重新获得了成骨细胞表型。临床、放射学和组织学数据表明,该模型与人类骨肉瘤的骨浓缩形式具有高度相似性。

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