Abstract

EMI Domain Containing 1 (EMID1) was identified as a potential candidate metastasis-promoting gene. We sought to clarify the molecular function of EMID1 and the protein expression. Overexpression and knockdown studies using mouse tumor cell lines identified two novel functions of EMID1: intracellular signaling involving enhancement of cell growth via cell cycle promotion and suppression of cell motility, and inhibition of cell–matrix adhesion by extracellularly secreted EMID1. EMID1 deposited on the culture dish induced self-detachment of cells that overexpressed the protein and inhibited adhesion of additionally seeded cells. This multifunctional property involving both intracellular signaling and the extracellular matrix suggests that EMID1 may be a matricellular proteins. Expression analysis using immunohistochemical staining revealed expression of EMID1 that was limited to chief cells of the gastric fundic gland and β cells of the pancreatic islets in normal adult human tissues, implying cell-specific functions of this molecule. In addition, increased expression of EMID1 protein detected in some cases of human cancers implies that EMID1 might be a new therapeutic target for cancer treatment.

Highlights

  • EMI Domain Containing 1 (EMID1) was identified as a potential candidate metastasis-promoting gene

  • EMID1 is a candidate metastasis-promoting molecule identified by expression analysis using the mouse metastasis model s­ystem[1,4]

  • We identified some unique features of EMID1, which has been identified as a candidate molecule for promoting cancer metastasis in the murine model

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Summary

Introduction

EMI Domain Containing 1 (EMID1) was identified as a potential candidate metastasis-promoting gene. EMID1 deposited on the culture dish induced self-detachment of cells that overexpressed the protein and inhibited adhesion of seeded cells. This multifunctional property involving both intracellular signaling and the extracellular matrix suggests that EMID1 may be a matricellular proteins. There are some reports of comprehensive analysis of gene mutations and expression profiles in human cancers demonstrated that EMID1 is a potential candidate molecule associated with development or metastasis of cancers, but its molecular mechanism has not been ­clarified[6,7,8]. We aimed to clarify the distribution of EMID1 expression in adult human normal and cancer tissues. We present here the unique functions of EMID1 protein and its association with cancer metastasis

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