Gill Heart Institute and Division of Cardiovascular Medicine, University of Kentucky, 740 S. Limestone Street, Lexington, KY 40536-0200, USA.
Exp Hematol. 2010 Dec;38(12):1131-1142.e1. doi: 10.1016/j.exphem.2010.08.003. Epub 2010 Aug 26.
The ischemic myocardium releases multiple chemotactic factors responsible for the mobilization and recruitment of bone marrow-derived cells to injured myocardium. However, the mobilization of primitive pluripotent stem cells (PSCs) enriched in very small embryonic-like stem cells (VSELs) in various cardiac ischemic scenarios is not well understood.
Fifty-four ischemic heart disease patients, including subjects with stable angina, non-ST elevation myocardial infarction, and ST elevation myocardial infarction (STEMI) and 12 matched controls were enrolled. The absolute numbers of circulating stem/primitive cells in samples of peripheral blood (PB) were quantitated by ImageStream analysis and conventional flow cytometry. Gene expression of PSC (Oct-4 and Nanog), early cardiomyocyte (Nkx-2.5 and GATA-4), and endothelial (von Willebrand factor) markers was analyzed by real-time polymerase chain reaction.
The absolute numbers of PSCs, stem cell populations enriched in VSELs, and hematopoietic stem cells present in PB were significantly higher in STEMI patients at presentation and declined over time. There was a corresponding increase in pluripotent, cardiac, and endothelial gene expression in unfractionated PB cells and sorted PB-derived primitive CD34(+) cells. The absolute numbers of circulating VSELs and hematopoietic stem cells in STEMI correlated negatively with patient age.
Myocardial ischemia mobilizes primitive PSCs including pluripotent VSELs into the circulation. The peak of mobilization occurs within 12 hours in patients presenting with STEMI, which may represent a therapeutic window for future clinical applications. Reduced stem cell mobilization with advancing age could explain, in part, the observation that age is associated with poor prognosis in patients with myocardial infarction.
缺血心肌释放多种趋化因子,负责动员和募集骨髓源性细胞到损伤的心肌。然而,在各种心脏缺血情况下,原始多能干细胞(PSCs)的动员,其中富含非常小的胚胎样干细胞(VSELs),还不太清楚。
54 例缺血性心脏病患者,包括稳定型心绞痛、非 ST 段抬高型心肌梗死和 ST 段抬高型心肌梗死(STEMI)患者和 12 例匹配的对照者纳入研究。通过流式细胞术和 ImageStream 分析对周围血(PB)样本中循环干细胞/原始细胞的绝对数量进行定量。通过实时聚合酶链反应分析 PSC(Oct-4 和 Nanog)、早期心肌细胞(Nkx-2.5 和 GATA-4)和内皮细胞(von Willebrand 因子)标志物的基因表达。
在发病时和发病后 STEMI 患者的 PB 中,PSCs、富含 VSELs 的干细胞群体和造血干细胞的绝对数量明显更高,且随时间下降。未分离的 PB 细胞和分选的 PB 来源的原始 CD34(+)细胞中出现多能性、心脏和内皮基因表达的相应增加。循环 VSELs 和造血干细胞的绝对数量与 STEMI 患者的年龄呈负相关。
心肌缺血将原始 PSCs 包括多能性 VSELs 动员到循环中。动员的高峰发生在 STEMI 患者发病后 12 小时内,这可能代表了未来临床应用的治疗窗。随着年龄的增长,干细胞动员减少,部分解释了年龄与心肌梗死患者预后不良相关的观察结果。
