| Literature DB >> 27619159 |
Sonia I Vlaicu1, Alexandru Tatomir2, Dallas Boodhoo3, Takahiro Ito3, Matthew Fosbrink3, Cornelia Cudrici3, Armugam P Mekala2, Jonathan Ciriello3, Doiniţa Crişan4, Emil Boţan4, Violeta Rus5, Horea Rus6.
Abstract
The complement system is an important player in the development of atherosclerosis. Previously reported as a cell cycle regulator, RGC-32 is an essential effector of the terminal complement complex, C5b-9. In this study, our aims were to determine the expression of RGC-32 in the human atherosclerotic arterial wall and to delineate the mechanisms through which RGC-32 affects C5b-9-induced endothelial cell proliferation and migration. We now demonstrate that RGC-32 is expressed in human aortic atherosclerotic wall and that RGC-32 expression increases with the progression of atherosclerosis. Furthermore, silencing of RGC-32 expression abolished C5b-9-induced human aortic endothelial cell (HAEC) proliferation and migration. Of the 279 genes differentially expressed in HAECs after RGC-32 silencing, the genes involved in cell adhesion and cell cycle activation were significantly regulated by RGC-32. RGC-32 silencing caused a significant reduction in the expression of cyclin D1, cyclin D3, Akt, ROCK1, Rho GDP dissociation inhibitor alpha and profilin. These data suggest that RGC-32 mediates HAEC migration through the regulation of RhoA and ROCK1 expression and is involved in actin cytoskeletal organization. Thus, RGC-32 has promising therapeutic potential with regard to angiogenesis and atherosclerosis.Entities:
Keywords: Atherosclerosis; C5b-9; Endothelial cells; Migration; Proliferation; RGC-32
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Year: 2016 PMID: 27619159 DOI: 10.1016/j.yexmp.2016.09.004
Source DB: PubMed Journal: Exp Mol Pathol ISSN: 0014-4800 Impact factor: 3.362