Abstract
Tumor metastasis is the most common cause of cancer death. Elucidation of the mechanism of tumor metastasis is therefore important in the development of novel, effective anti-cancer therapies to reduce cancer mortality. Interaction between cancer cells and surrounding stromal cells in the tumor microenvironment is a key factor in tumor metastasis. Using a co-culture assay system with human prostate cancer LNCaP cells and primary human prostate stromal cells, we identified epithelial membrane protein 1 (EMP1) as a gene with elevated expression in the cancer cells. The orthotopic injection of LNCaP cells overexpressing EMP1 (EMP1-LNCaP cells) into the prostate of nude mice induced lymph node and lung metastases, while that of control LNCaP cells did not. EMP1-LNCaP cells had higher cell motility and Rac1 activity than control LNCaP cells. These results were also observed in other lines of cancer cells. We newly identified copine-III as an intracellular binding partner of EMP1. Knockdown of copine-III attenuated the increased cell motility and Rac1 activity in EMP1-LNCaP cells. Reduced cell motility and Rac1 activity following knockdown of copine-III in EMP1-LNCaP cells were recovered by re-expression of wild-type copine-III, but not of a copine-III mutant incapable of interacting with EMP1, suggesting the importance of the EMP1–copine-III interaction. Phosphorylated and activated Src and a Rac guanine nucleotide exchange factor Vav2 were found to be involved in the EMP1-induced enhancement of cell motility and Rac1 activation. Moreover, EMP1 was highly expressed in prostate cancer samples obtained from patients with higher Gleason score. These results demonstrate that upregulation of EMP1 significantly increases cancer cell migration that leads to tumor metastasis, suggesting that EMP1 may play an essential role as a positive regulator of tumor metastasis.
Highlights
Electronic supplementary material The online version of this article contains supplementary material, which is available to authorized users.Tumor metastasis is frequently observed in the course of malignant cancer progression and is the major lifethreatening event in individuals with cancer [1, 2]
To determine the underlying mechanism by which epithelial membrane protein 1 (EMP1) and copine-III promote cell migration, we examined Rac1 activity by the pull-down assay using glutathione beads bound to glutathione S-transferase (GST)-p21-activated kinase1 (PAK)-Cdc42 and Rac-binding domain (CRIB), as Rac1 essentially activates cell migration and cancer metastasis [19]
EMP1-related potentiation of tumor metastasis is supported by the finding that prostate cancer samples with higher Gleason score abundantly express EMP1, compared with those with lower Gleason score
Summary
Tumor metastasis is frequently observed in the course of malignant cancer progression and is the major lifethreatening event in individuals with cancer [1, 2]. In the initial stages of tumor metastasis, cancer cells escape from the originating tumor site and invade into the surrounding tissues in which stromal cells exist. The physical and functional contact between escaped cancer cells and stromal cells contributes to the formation and enlargement of the tumor microenvironment, leading to alterations in the characteristics of cancer cells. It has recently been considered that the tumor microenvironment is an important biological concept behind the mechanism of cancer progression including tumor growth, spread, and metastasis [3,4,5]. Clinical and experimental studies have provided evidence that chemical communication between cancer cells and the surrounding microenvironment through growth
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