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首页> 外文期刊>Current vascular pharmacology >Milk fat globule epidermal growth factor VIII signaling in arterial wall remodeling
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Milk fat globule epidermal growth factor VIII signaling in arterial wall remodeling

机译:乳脂球表皮生长因子VIII信号在动脉壁重塑中的信号转导

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Arterial inflammation and remodeling, important sequellae of advancing age, are linked to the pathogenesis of age-associated arterial diseases e.g. hypertension, atherosclerosis, and metabolic disorders. Recently, high-throughput proteomic screening has identified milk fat globule epidermal growth factor VIII (MFG-E8) as a novel local biomarker for aging arterial walls. Additional studies have shown that MFG-E8 is also an element of the arterial inflammatory signaling network. The transcription, translation, and signaling levels of MFG-E8 are increased in aged, atherosclerotic, hypertensive, and diabetic arterial walls in vivo as well as activated vascular smooth muscle cells (VSMC) and a subset of macrophages in vitro. In VSMC, MFG-E8 increases proliferation and invasion as well as the secretion of inflammatory molecules. In endothelial cells (EC), MFG-E8 facilitates apoptosis. In addition, MFG-E8 has been found to be an essential component of the endothelial-derived microparticles that relay biosignals and modulate arterial wall phenotypes. This review mainly focuses upon the landscape of MFG-E8 expression and signaling in adverse arterial remodeling. Recent discoveries have suggested that MFG-E8 associated interventions are novel approaches for the retardation of the enhanced rates of VSMC proliferation and EC apoptosis that accompany arterial wall inflammation and remodeling during aging and age-associated arterial disease.
机译:动脉炎症和重塑是年龄增长的重要后遗症,与年龄相关的动脉疾病(如高血压、动脉粥样硬化和代谢紊乱)的发病机制有关。最近,高通量蛋白质组学筛选已将乳脂球表皮生长因子 VIII (MFG-E8) 确定为动脉壁老化的新型局部生物标志物。其他研究表明,MFG-E8 也是动脉炎症信号网络的一个组成部分。MFG-E8 的转录、翻译和信号转导水平在体内老化、动脉粥样硬化、高血压和糖尿病动脉壁以及活化的血管平滑肌细胞 (VSMC) 和体外巨噬细胞亚群中增加。在VSMC中,MFG-E8增加增殖和侵袭以及炎症分子的分泌。在内皮细胞 (EC) 中,MFG-E8 促进细胞凋亡。此外,已发现 MFG-E8 是内皮衍生微粒的重要组成部分,可传递生物信号和调节动脉壁表型。本文主要关注MFG-E8在不良动脉重塑中的表达和信号转导。最近的发现表明,MFG-E8 相关干预措施是延缓衰老和年龄相关动脉疾病期间伴随动脉壁炎症和重塑的 VSMC 增殖和 EC 细胞凋亡率增强的新方法。

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