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在大鼠模型中,内皮祖细胞移植可改善心肌梗死后的新生血管形成及左心室功能。

Transplantation of endothelial progenitor cells improves neovascularization and left ventricular function after myocardial infarction in a rat model.

作者信息

Schuh Alexander, Liehn Elisa A, Sasse Alexander, Hristov Mihail, Sobota Radoslaw, Kelm Malte, Merx Marc W, Weber Christian

机构信息

IZKF "BIOMAT", Aachen, Germany.

出版信息

Basic Res Cardiol. 2008 Jan;103(1):69-77. doi: 10.1007/s00395-007-0685-9. Epub 2007 Nov 12.

Abstract

Cell transplantation has recently emerged as a novel therapy for ischemic heart disease. The presented study investigated the effect of intramyocardial transfer of human endothelial progenitor cells (EPCs) and stromal-cell derived factor-1alpha (SDF-1alpha) on left ventricular function in a chronic setting after myocardial infarction in cyclosporine treated rats. BrdU-labeled EPCs (10(6)), 10 microg SDF-1alpha, EPCs+SDF-1alpha or placebo medium were injected directly into the border infarct zone 4 weeks after acute myocardial infarction. Eight weeks after transplantation, echocardiography identified significantly improved fractional shortening after EPC or EPCs+SDF-1alpha injection as compared with injection of placebo medium. Investigating isolated hearts revealed a significant increase in left ventricular developing pressure after transplantation of SDF-1alpha or EPCs+SDF-1alpha. Furthermore, coronary flow rates were significantly elevated, especially after transplantation of EPCs+SDF-1alpha (under catecholamine stress 24.2 +/- 1.55 ml/min vs. 13.1 +/- 1 ml/min in the control) correlating with increased density of CD31+ vessel structures in the EPC as well as EPCs+SDF-1alpha groups, thus defining a higher rate of neovascularization. Notably, SDF-1alpha injected hearts showed only a trend towards improvement in coronary flow. BrdU+ signals were detected in infarct areas, partially integrating into vascular networks. The rate of apoptotic cells as well as the amount of inflammatory cells was significantly elevated in the placebo control group. In conclusion, transplantation of EPCs as well as EPCs+SDF-1alpha associated with improvement in cardiac function after infarction, which was attributable to enhanced neovascularization and decreased inflammation. These results imply a combined benefit of EPCs+SDF-1alpha in the treatment of myocardial infarction.

摘要

细胞移植最近已成为治疗缺血性心脏病的一种新疗法。本研究调查了在环孢素处理的大鼠心肌梗死后的慢性情况下,人内皮祖细胞(EPCs)和基质细胞衍生因子-1α(SDF-1α)心肌内移植对左心室功能的影响。急性心肌梗死后4周,将BrdU标记的EPCs(10⁶个)、10微克SDF-1α、EPCs+SDF-1α或安慰剂介质直接注射到梗死边缘区。移植后8周,超声心动图显示,与注射安慰剂介质相比,注射EPCs或EPCs+SDF-1α后,缩短分数显著改善。对离体心脏的研究显示,移植SDF-1α或EPCs+SDF-1α后,左心室舒张末压显著升高。此外,冠状动脉血流速度显著升高,尤其是在移植EPCs+SDF-1α后(在儿茶酚胺应激下为24.2±1.55毫升/分钟,而对照组为13.1±1毫升/分钟),这与EPCs组和EPCs+SDF-1α组中CD31+血管结构密度增加相关,从而确定了更高的新生血管形成率。值得注意 的是,注射SDF-1α的心脏仅显示出冠状动脉血流改善的趋势。在梗死区域检测到BrdU+信号,部分整合到血管网络中。安慰剂对照组中凋亡细胞率和炎症细胞数量显著升高。总之,EPCs以及EPCs+SDF-1α移植与梗死后心脏功能改善相关,这归因于新生血管形成增强和炎症减少。这些结果表明 EPCs+SDF-1α在治疗心肌梗死方面具有联合益处。

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