Zenovich Andrey G, Taylor Doris A
Center for Cardiovascular Repair, University of Minnesota, Minneapolis, MN 55455, USA.
Front Biosci. 2008 May 1;13:3621-36. doi: 10.2741/2954.
As coronary artery disease (CAD) continues to be the primary cause of mortality, a more in-depth understanding of pathophysiology and novel treatments are being sought. The past two decades have established inflammation as a driving force behind CAD--from endothelial dysfunction to heart failure. Recent advances in stem/progenitor cell biology have led to initial applications of progenitor cells in CAD continuum and have revealed that atherosclerosis is, at least in part, a disease of failed endogenous vascular repair. Several key progenitor cell populations including endothelial progenitor cells (AC133+/CD34+ population), vascular progenitors (CD31+/CD45(low) population), KDR+ cells and other bone marrow subtypes are mobilized for vascular repair. However, age and risk factors negatively impact these cells even prior to clinical CAD. Sex-based differences in progenitor cell capacity for repair have emerged as a new research focus that may offer mechanistic insights into clinical CAD discrepancies between men and women. Quantifying injury and cell-based repair and better defining their interactions should enable us to halt or even prevent CAD by enhancing the repair side of the repair/injury equation.
由于冠状动脉疾病(CAD)仍然是主要的死亡原因,人们正在寻求对其病理生理学有更深入的了解以及新的治疗方法。在过去的二十年里,炎症已被确认为CAD背后的驱动力——从内皮功能障碍到心力衰竭。干细胞/祖细胞生物学的最新进展已导致祖细胞在CAD连续过程中的初步应用,并揭示动脉粥样硬化至少部分是一种内源性血管修复失败的疾病。包括内皮祖细胞(AC133+/CD34+群体)、血管祖细胞(CD31+/CD45(低)群体)、KDR+细胞和其他骨髓亚型在内的几个关键祖细胞群体被动员起来进行血管修复。然而,即使在临床CAD出现之前,年龄和危险因素就会对这些细胞产生负面影响。祖细胞修复能力的性别差异已成为一个新的研究重点,这可能为男女临床CAD差异提供机制性见解。量化损伤和基于细胞的修复,并更好地定义它们之间的相互作用,应该能使我们通过增强修复/损伤平衡中的修复方面来阻止甚至预防CAD。
