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Activated Ras alters lens and corneal development through induction of distinct downstream targets
Authors:Daniel Burgess  Yan Zhang  Ed Siefker  Ryan Vaca  Murali R Kuracha  Lixing Reneker  Paul A Overbeek  Venkatesh Govindarajan
Affiliation:(1) Department of Surgery, Creighton University, 2500 California Plaza, 68178 Omaha, NE, USA;(2) Department of Ophthalmology, University of Missouri School of Medicine, 65212 Columbia, MO, USA;(3) Department of Molecular & Cellular Biology, Baylor College of Medicine, 77030 Houston, TX, USA
Abstract:

Background  

Mammalian Ras genes regulate diverse cellular processes including proliferation and differentiation and are frequently mutated in human cancers. Tumor development in response to Ras activation varies between different tissues and the molecular basis for these variations are poorly understood. The murine lens and cornea have a common embryonic origin and arise from adjacent regions of the surface ectoderm. Activation of the fibroblast growth factor (FGF) signaling pathway induces the corneal epithelial cells to proliferate and the lens epithelial cells to exit the cell cycle. The molecular mechanisms that regulate the differential responses of these two related tissues have not been defined. We have generated transgenic mice that express a constitutively active version of human H-Ras in their lenses and corneas.
Keywords:
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