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C-甲硫氨酸激活对于B16小鼠黑色素瘤细胞在肝脏定植是必要的,但并不充分。

C-met activation is necessary but not sufficient for liver colonization by B16 murine melanoma cells.

作者信息

Lin S, Rusciano D, Lorenzoni P, Hartmann G, Birchmeier W, Giordano S, Comoglio P, Burger M M

机构信息

Friedrich Miescher Institut, Basel, Switzerland.

出版信息

Clin Exp Metastasis. 1998 Apr;16(3):253-65. doi: 10.1023/a:1006596909948.

Abstract

Metastasis to the liver is a frequent event in clinical oncology, the molecular mechanisms of which are not fully understood. We have recently reported a consistent overexpression of c-met in B16 melanoma cells selected in vivo for enhanced liver metastatic ability. In this study we address the question as to whether constitutive activation of c-met is a necessary and sufficient condition for enhanced liver colonization by B16 melanoma cells. Different levels of c-met expression and/or activation in B16 cells were achieved by subcloning, or by c-DNA transfection with either HGF/SF or the oncogenic form of c-met (tpr-met). Metastatic ability of the different populations was then evaluated in vivo by the lung colonization (experimental metastasis) assay. Results indicate that c-met (but not tpr-met) activation in B16 melanoma cells may increase their liver colonizing potential, probably by enhancing motility and invasion in response to paracrine interactions with its ligand. C-met expression per se, however, is not able to change the organ specificity of the cells. C-met activation appears instead to be required at later stages of liver colonization by B16 melanoma cells, in order to enhance their site-specific metastatic ability.

摘要

肝脏转移是临床肿瘤学中常见的现象,其分子机制尚未完全明确。我们最近报道,在体内筛选出的具有增强肝脏转移能力的B16黑色素瘤细胞中,c-met持续过表达。在本研究中,我们探讨了c-met的组成性激活是否是B16黑色素瘤细胞增强肝脏定植的必要和充分条件。通过亚克隆,或用HGF/SF或c-met的致癌形式(tpr-met)进行cDNA转染,在B16细胞中实现了不同水平的c-met表达和/或激活。然后通过肺定植(实验性转移)试验在体内评估不同群体的转移能力。结果表明,B16黑色素瘤细胞中c-met(而非tpr-met)的激活可能会增加其肝脏定植潜力,这可能是通过增强对其配体的旁分泌相互作用的运动性和侵袭性来实现的。然而,c-met的表达本身并不能改变细胞的器官特异性。相反,c-met激活似乎是B16黑色素瘤细胞肝脏定植后期所必需的,以增强其位点特异性转移能力。

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