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循环血管生成细胞的分离

Isolation of circulating angiogenic cells.

作者信息

Vaughan Erin E, O'Brien Timothy

机构信息

Regenerative Medicine Institute, University College Hospital, National University of Ireland, Galway, Ireland.

出版信息

Methods Mol Biol. 2012;916:351-6. doi: 10.1007/978-1-61779-980-8_25.

Abstract

Endothelial progenitor cells (EPCs) were first identified by Ashara et al. in 1997 (Asahara et al. Science 275:964-967, 1997) and were thought to contribute to angiogenesis and vasculogenesis. Since their discovery, circulating levels of EPCs were found to serve as biomarkers as low levels correlate with increased cardiovascular events and death from cardiovascular causes (Werner et al. N Engl J Med 353:999-1007, 2005; Fadini et al. J Am Coll Cardiol 45:1449-1457, 2005; Hill et al. N Engl J Med 348:593-600, 2003; Schmidt-Lucke et al. Circulation 111:2981-2987, 2005). Additionally, EPC dysfunction has been associated with diabetes mellitus and other disease states. However, recently there has been a great deal of controversy in the field over the exact definition and function of an EPC. To help classify EPCs, they have been divided into two distinct groups (1) circulating angiogenic cells (also referred to as early EPCs) and (2) endothelial colony forming cells (also referred to as late outgrowth EPCs). Circulating angiogenic cells are believed to represent a cell population enriched in monocytes and exert their angiogenic effects via paracrine and signaling mechanisms whereas endothelial colony forming cells are true EPCs and may enhance angiogenesis and vasculogenesis by incorporating into the newly forming vessels. Here the isolation and identification of circulating angiogenic cells are described.

摘要

内皮祖细胞(EPCs)于1997年首次由朝原等人鉴定(朝原等人,《科学》275:964 - 967,1997年),被认为有助于血管生成和血管发生。自发现以来,EPCs的循环水平被发现可作为生物标志物,因为低水平与心血管事件增加和心血管原因导致的死亡相关(维尔纳等人,《新英格兰医学杂志》353:999 - 1007,2005年;法迪尼等人,《美国心脏病学会杂志》45:1449 - 1457,2005年;希尔等人,《新英格兰医学杂志》348:593 - 600,2003年;施密特 - 卢克等人,《循环》111:2981 - 2987,2005年)。此外,EPC功能障碍与糖尿病和其他疾病状态有关。然而,最近该领域对于EPC的确切定义和功能存在大量争议。为了帮助对EPC进行分类,它们被分为两个不同的组:(1)循环血管生成细胞(也称为早期EPCs)和(2)内皮集落形成细胞(也称为晚期扩增EPCs)。循环血管生成细胞被认为代表富含单核细胞的细胞群体,并通过旁分泌和信号传导机制发挥其血管生成作用,而内皮集落形成细胞是真正的EPCs,可能通过整合到新形成的血管中来增强血管生成和血管发生。本文描述了循环血管生成细胞的分离和鉴定。

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