Green Tea Induces Annexin-I Expression in Human Lung Adenocarcinoma A549 Cells: Involvement of Annexin-I in Actin Remodeling
Penn collection
Degree type
Discipline
Subject
Cell migration
Chemoprevention
F-actin
Green tea
Lung adenocacinoma MeSH: Actins
Adenocarcinoma
Annexin A1
Anticarcinogenic Agents
Camellia sinensis
Cell Adhesion
Cell Line
Tumor
Cell Movement
Dose-Response Relationship
Drug
Gene Expression
Humans
Lung Neoplasms
Plant Extracts
Polymers
Proteomics
RNA
Messenger EMTREE drug terms: actin
green tea extract
lipocortin 1 EMTREE medical terms: actin polymerization
article
cell adhesion
cell motility
controlled study
dose response
human
human cell
lung adenocarcinoma
priority journal
protein expression
transcription regulation
Dentistry
Oral Biology and Oral Pathology
Periodontics and Periodontology
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Abstract
Green tea polyphenols exhibit multiple antitumor activities in various in vitro and in vivo tumor models, and the mechanisms of action are not clear. Previously, we found that green tea extract (GTE) regulates actin remodeling in different cell culture systems. Actin remodeling plays an important role in cancer cell morphology, cell adhesion, motility, and invasion. Using proteomic approaches, we found GTE-induced expression of annexin-I, a multifunctional actin binding protein, in these cell lines. In this study, we aimed to further define the functional role of GTE-induced annexin-I expression in actin remodeling, cell adhesion, and motility in lung adenocarcinoma A549 cells. We found that GTE stimulates the expression of annexin-I in a dose-dependent fashion. The GTE-induced annexin-I expression appears to be at the transcription level, and the increased annexin-I expression mediates actin polymerization, resulting in enhanced cell adhesion and decreased motility. Annexin-I specific interference resulted in loss of GTE-induced actin polymerization and cell adhesion, but not motility. In fact, annexin-I specific interference itself inhibited motility even without GTE. Together, annexin-I plays an important role in GTE-induced actin remodeling, and it may serve as a potential molecular target associated with the anticancer activities of green tea. © 2007 USCAP, Inc All rights reserved.