Author: Huang CW, Chen HY, Yen MH, Chen JJ, Young TH, Cheng JY.
Affiliation: Institute of Biomedical Engineering, National Taiwan University, Taipei, Taiwan.
Conference/Journal: PLoS One.
Date published: 2011
Other:
Volume ID: 6 , Issue ID: 10 , Pages: e25928 , Word Count: 271
BACKGROUND:
Electrotaxis is the movement of adherent living cells in response to a direct current (dc) electric field (EF) of physiological strength. Highly metastatic human lung cancer cells, CL1-5, exhibit directional migration and orientation under dcEFs. To understand the transcriptional response of CL1-5 cells to a dcEF, microarray analysis was performed in this study.
METHODOLOGY/PRINCIPAL FINDINGS:
A large electric-field chip (LEFC) was designed, fabricated, and used in this study. CL1-5 cells were treated with the EF strength of 0 mV/mm (the control group) and 300 mV/mm (the EF-treated group) for two hours. Signaling pathways involving the genes that expressed differently between the two groups were revealed. It was shown that the EF-regulated genes highly correlated to adherens junction, telomerase RNA component gene regulation, and tight junction. Some up-regulated genes such as ACVR1B and CTTN, and some down-regulated genes such as PTEN, are known to be positively and negatively correlated to cell migration, respectively. The protein-protein interactions of adherens junction-associated EF-regulated genes suggested that platelet-derived growth factor (PDGF) receptors and ephrin receptors may participate in sensing extracellular electrical stimuli. We further observed a high percentage of significantly regulated genes which encode cell membrane proteins, suggesting that dcEF may directly influence the activity of cell membrane proteins in signal transduction.
CONCLUSIONS/SIGNIFICANCE:
In this study, some of the EF-regulated genes have been reported to be essential whereas others are novel for electrotaxis. Our result confirms that the regulation of gene expression is involved in the mechanism of electrotactic response.
PMID: 21998723 [PubMed - indexed for MEDLINE] PMCID: PMC3187831
full article: http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3187831/