Overexpression of Vimentin Contributes to Prostate Cancer Invasion and Metastasis Via Src Regulation

Overview

Journal Anticancer Res

Specialty Oncology

Date 2008 Apr 4

PMID 18383865

Citations 84

Authors

Juncheng Wei

Gang Xu

Mingfu Wu

Yongtao Zhang

Qiong Li

Ping Liu

Tao Zhu

Anping Song

Liangpin Zhao

Zhiqiang Han

Gang Chen

Li Meng

Jianfeng Zhou

Yunping Lu

Shixuan Wang

Ding Ma

Affiliations

Soon will be listed here.

Abstract

A significant proportion of prostate cancer patients treated with curative intent develop advanced disease. At a fundamental biological level, very little is known about what makes the disease aggressive and metastatic. Observational pathology reports and experimental data suggest that an epithelial-mesenchymal transition (EMT) is involved in prostate cancer invasiveness. The mechanism by which vimentin promotes prostate cancer cell invasion and metastasis was examined. The highly metastatic human prostate epithelial cell line PC-3M-1E8 (1E8-H) and the low metastatic line PC-3M-2B4 (2B4-L) were used for comparative proteomic analysis by two-dimensional gel electrophoresis, followed by matrix-assisted laser desorption/time of flight mass spectrometry (MALDI-TOF-MS). A transwell assay was performed to test cell migration and invasion and immunoblotting was used to analyze the relative expression of proteins. High vimentin expression was detected in 1E8-H compared to 2B4-L cells. Down-regulation of vimentin in 1E8-H by antisense-vimentin transfection led to a significant inhibition of invasiveness, and selective stimulation of vimentin activity in 2B4-L by delivery of recombinant vimentin promoted cell invasiveness. Vimentin activity was associated with C-src, beta-catenin and E-cadherin expression. PP2, a specific inhibitor of src family kinases, reduced phospho-beta-catenin expression and induce E-cadherin expression. Vimentin promotes tumor cell invasiveness and the targeting of vimentin/C-src may be a promising strategy for preventing or blocking prostate cancer metastasis.

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