| Literature DB >> 26091721 |
Sonia I Vlaicu1,2, Alexandru Tatomir1, Violeta Rus3, Armugam P Mekala1,4, Petru A Mircea2, Florin Niculescu3, Horea Rus5,6,7.
Abstract
The pathogenesis of atherosclerotic inflammation is a multi-step process defined by the interweaving of excess modified lipid particles, monocyte-macrophages populations, and innate immune and adaptive immunity effectors. A part of innate immunity, the complement system, is an important player in the induction and progression of atherosclerosis. The accumulation of either oxidized or enzymatically modified LDL-bound to C-reactive protein or not-prompts complement activation leading to the assembly of the terminal complement C5b-9 complex in the atherosclerotic lesion. The sublytic C5b-9 assembly leads to the activation and proliferation of smooth muscle and endothelial cells, accompanied by the release of various chemotactic, pro-adhesion, and procoagulant cytokines from these cells. Response gene to complement (RGC)-32, an essential effector of the terminal complement complex C5b-9, also affects atherogenesis, propelling vascular smooth muscle cell proliferation and migration, stimulating endothelial proliferation, and promoting vascular lesion formation. A substantial amount of experimental work has suggested a role for the complement system activation during atherosclerotic plaque formation, with the proximal classical complement pathway seemingly having a protective effect and terminal complement contributing to accelerated atherogenesis. All these data suggest that complement plays an important role in atherogenesis.Entities:
Keywords: Atherosclerosis; C5b-9 complement complex; Complement activation; Endothelial cells; RGC-32; Smooth muscle cells
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Year: 2016 PMID: 26091721 DOI: 10.1007/s12026-015-8669-6
Source DB: PubMed Journal: Immunol Res ISSN: 0257-277X Impact factor: 2.829