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Excess FGF-7 in corneal epithelium causes corneal intraepithelial neoplasia in young mice and epithelium hyperplasia in adult mice
Journal
American Journal of Pathology
Journal Volume
172
Journal Issue
3
Pages
638-649
Date Issued
2008
Author(s)
Abstract
We hypothesized that human ocular surface squamous neoplasia (OSSN) may result from the continuous growth stimulation of corneal epithelial progenitor cells. In the present study, we analyzed the effects of excess fibroblast growth factor-7 (FGF-7) on both the proliferation and differentiation of corneal epithelium in a novel Krt12-rtTA/tet-O-FGF-7 double transgenic mouse model in which cornea-specific FGF-7 overexpression is achieved by doxycycline (Dox) treatment. When such adult mice were exposed to Dox, they exhibited epithelial hyperplasia with increases in phospho-extracellular signal-regulated kinase 1/2-, nuclear β-catenin-, and 5-bromo-2′-adeoxyuridine-labeled cells and altered keratin (K) 14 (K14) expression pattern, a normal K12 expression pattern, and the normal absence of K10. Hyperplasia of the adult cornea was fully reversible 2 weeks after the removal of Dox from chow. In contrast, double transgenic embryos that were exposed to Dox from embryonic day 0.5 to postnatal day 21 developed papillomatous tumors in the cornea, resembling human OSSN, and ectopic gland-like structures in the limbus, accompanied by the down-regulation of K12 and the up-regulation of K14, Pax6, and p63. These epithelial anomalies observed in young experimental mice were not fully resolved after the termination of Dox induction. Taken together, Krt12-rtTA/tet-O-FGF-7 mice may be a suitable animal model for the study of the molecular and cellular mechanisms of human OSSN. Copyright ? American Society for Investigative Pathology.
SDGs
Other Subjects
beta catenin; broxuridine; cytokeratin 14; doxycycline; keratinocyte growth factor; mitogen activated protein kinase 1; mitogen activated protein kinase 3; animal experiment; animal model; animal tissue; article; cell differentiation; cell proliferation; controlled study; cornea; cornea disease; cornea epithelium; cornea limbus; down regulation; epithelium hyperplasia; female; immunohistochemistry; mouse; nonhuman; ocular surface squamous neoplasia; perinatal period; priority journal; protein expression; stem cell; transgenic mouse; upregulation; Western blotting
Publisher
American Society for Investigative Pathology Inc.
Type
journal article