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自分泌肝细胞生长因子/分散因子- Met信号通路诱导C127细胞发生转化并呈现侵袭/转移表型。

Autocrine hepatocyte growth factor/scatter factor-Met signaling induces transformation and the invasive/metastastic phenotype in C127 cells.

作者信息

Jeffers M, Rong S, Anver M, Vande Woude G F

机构信息

ABL-Basic Research Program, NCI-Frederick Cancer Research and Development Center, Frederick, Maryland 21702, USA.

出版信息

Oncogene. 1996 Aug 15;13(4):853-6.

PMID:8761307
Abstract

Hepatocyte growth factor/scatter factor (HGF/SF) is a pleiotropic effector of cells expressing the Met tyrosine kinase receptor. C127 is a non-tumorigenic mouse cell line which expresses negligible levels of HGF/SF and Met proteins. In the present report we have generated C127 cells which overexpress HGF/SF and/or Met proteins, and have analysed the effect of HGF/SF-Met signaling in these cells. We show that this signaling pathway stimulates the growth and invasiveness of C127 cells in vitro and that cells overexpressing both HGF/SF and Met proteins (but neither alone) are phenotypically transformed and highly tumorigenic and metastatic in vivo. Our data unequivocally demonstrates the autocrine dependency of HGF/SF-Met-induced transformation and metastasis in this system and supports the theory that the inappropriate expression of HGF/SF and Met proteins could play a role in the development and spread of human tumors. In addition, this system may be useful for identifying metastasis-associated genes that are activated by HGF/SF-Met signaling.

摘要

肝细胞生长因子/分散因子(HGF/SF)是一种对表达Met酪氨酸激酶受体的细胞具有多效性作用的效应因子。C127是一种非致瘤性小鼠细胞系,其HGF/SF和Met蛋白表达水平极低。在本报告中,我们构建了过表达HGF/SF和/或Met蛋白的C127细胞,并分析了HGF/SF-Met信号在这些细胞中的作用。我们发现,该信号通路在体外刺激C127细胞的生长和侵袭,并且过表达HGF/SF和Met蛋白的细胞(而非单独过表达其中一种蛋白的细胞)在体内发生表型转化,具有高度致瘤性和转移性。我们的数据明确证明了该系统中HGF/SF-Met诱导的转化和转移存在自分泌依赖性,并支持HGF/SF和Met蛋白的异常表达可能在人类肿瘤发生和扩散中起作用这一理论。此外,该系统可能有助于鉴定由HGF/SF-Met信号激活的转移相关基因。

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