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血行转移的非侵袭性途径:一种新的小鼠乳腺肿瘤模型。

An invasion-independent pathway of blood-borne metastasis: a new murine mammary tumor model.

作者信息

Sugino Takashi, Kusakabe Takashi, Hoshi Nobuo, Yamaguchi Tomiko, Kawaguchi Takanori, Goodison Steve, Sekimata Masayuki, Homma Yoshimi, Suzuki Toshimitsu

机构信息

Department of Pathology, School of Medicine, Fukushima Medical University, Fukushima City, Japan.

出版信息

Am J Pathol. 2002 Jun;160(6):1973-80. doi: 10.1016/S0002-9440(10)61147-9.

Abstract

It is generally believed that active invasion by cancer cells is essential to the metastatic process. In this report, we describe a murine mammary tumor (MCH66) model of metastasis that does not require invasion into the vascular wall of both the primary tumor and the target organ, in this case, the lung. The process involves intravasation of tumor nests surrounded by sinusoidal blood vessels, followed by intravascular tumor growth in the lung, without penetration of the vascular wall during the process. Comparative studies using a nonmetastatic MCH66 clone (MCH66C8) and another highly invasive metastatic cell line (MCH416) suggested that high angiogenic activity and sinusoidal remodeling of tumor blood vessels were prerequisites for MCH66 metastasis. Differential cDNA analysis identified several genes that were overexpressed by MCH66, including genes for the angiogenesis factor pleiotrophin, and extracellular matrix-associated molecules that may modulate the microenvironment toward neovascularization. Our analyses suggest that tumor angiogenesis plays a role in the induction of invasion-independent metastasis. This model should prove useful in screening and development of new therapeutic agents for cancer metastasis.

摘要

一般认为,癌细胞的主动侵袭对于转移过程至关重要。在本报告中,我们描述了一种转移性小鼠乳腺肿瘤(MCH66)模型,该模型在原发性肿瘤和靶器官(在本病例中为肺)均不需要侵袭血管壁。该过程包括被窦状血管包围的肿瘤巢进入血管,随后肿瘤在肺内血管中生长,在此过程中血管壁未被穿透。使用非转移性MCH66克隆(MCH66C8)和另一种高侵袭性转移细胞系(MCH416)进行的比较研究表明,肿瘤血管的高血管生成活性和窦状重塑是MCH66转移的先决条件。差异cDNA分析鉴定了几个由MCH66过度表达的基因,包括血管生成因子多效生长因子的基因,以及可能调节微环境向新血管形成方向发展的细胞外基质相关分子。我们的分析表明,肿瘤血管生成在非侵袭性转移的诱导中起作用。该模型应被证明在筛选和开发用于癌症转移的新治疗药物方面有用。

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