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在原发性肿瘤生长的特定时间评估转移能力:一种新型的自发转移检测方法。

Evaluation of metastatic ability at specific times during primary tumor growth: a novel spontaneous metastasis assay.

作者信息

Takiguchi Y, Kuriyama T, Miyamoto T

机构信息

National Institute of Radiological Sciences Hospital, Chiba, Japan.

出版信息

Clin Exp Metastasis. 1995 May;13(3):184-90. doi: 10.1007/BF00132206.

DOI:10.1007/BF00132206
PMID:7750205
Abstract

A transformed NIH 3T3 fibroblast cell line, Cl-e, normally does not produce spontaneous metastasis from subcutaneous or footpad tumors in nude mice. However, pulmonary tumor nodules are formed when more than 1 x 10(3) cells are injected intravenously into nude mice. Co-injection of 1 x 10(6) heavily irradiated and inactivated cells increases the clonogenic ability of the viable cells in that tumor colonies then occur with as few as 1 x 10(2) viable cells. Utilizing the action of these inactivated cells to enhance the lung colonizing ability of a relatively small number of viable tumor cells, we have developed a novel experimental model of spontaneous metastasis. In this model, a footpad tumor of the nude mouse metastasizes to the lungs following intravenous injection of 1 x 10(6) inactivated cells at a specific time of tumor growth and following tumor foot amputation, whereas no spontaneous metastasis develops without injection of inactivated cells. This model enables us to detect metastatic ability which would otherwise be too low to detect using other assays. In addition, it allows us to evaluate metastatic ability at a specific time point during primary tumor growth, since no metastases can develop during the periods before inactivated cell injection and after tumor amputation. Using this model, we have determined that the metastatic ability of Cl-e tumors in the footpad is constant throughout the exponential and stationary growth phases, even though cells isolated from exponentially growing tumors possess a 3.3-fold greater lung colonizing ability following intravenous injection than those from stationary tumors. This new experimental model may be applicable to other tumor cell lines and to other analyses where metastatic ability during a defined interval of tumor growth is of importance.

摘要

一种转化的NIH 3T3成纤维细胞系Cl-e,通常不会在裸鼠的皮下或足垫肿瘤中自发转移。然而,当将超过1×10³个细胞静脉注射到裸鼠体内时,会形成肺肿瘤结节。共同注射1×10⁶个经过大量辐照并灭活的细胞可提高活细胞的克隆形成能力,因为此时只需1×10²个活细胞就能形成肿瘤集落。利用这些灭活细胞的作用来增强相对少量活肿瘤细胞的肺定植能力,我们开发了一种新型的自发转移实验模型。在这个模型中,在肿瘤生长的特定时间,对裸鼠的足垫肿瘤进行截肢后,静脉注射1×10⁶个灭活细胞,足垫肿瘤会转移到肺部,而不注射灭活细胞则不会发生自发转移。这个模型使我们能够检测到原本因太低而无法用其他检测方法检测到的转移能力。此外,它还使我们能够在原发性肿瘤生长的特定时间点评估转移能力,因为在注射灭活细胞之前和肿瘤截肢之后的时间段内不会发生转移。使用这个模型我们已经确定,Cl-e足垫肿瘤的转移能力在指数生长阶段和稳定生长阶段都是恒定的,尽管从指数生长的肿瘤中分离出的细胞在静脉注射后比从稳定期肿瘤中分离出的细胞具有高3.3倍的肺定植能力。这个新的实验模型可能适用于其他肿瘤细胞系以及其他在肿瘤生长的特定时间段内转移能力很重要的分析。

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