CCN1 promotes the differentiation of endothelial progenitor cells and reendothelialization in the early phase after vascular injury

被引:0
|
作者
Yang Yu
Yu Gao
Jun Qin
Chun-Yan Kuang
Ming-Bao Song
Shi-Yong Yu
Bin Cui
Jian-Fei Chen
Lan Huang
机构
[1] Institute of Cardiovascular Diseases,Department of Rehabilitation
[2] Xinqiao Hospital,undefined
[3] Third Military Medical University,undefined
[4] Southwest Hospital,undefined
[5] Third Military Medical University,undefined
来源
Basic Research in Cardiology | 2010年 / 105卷
关键词
Stem cells; Gene array; Endothelial cell differentiation; Matricellular genes;
D O I
暂无
中图分类号
学科分类号
摘要
Endothelial progenitor cells (EPCs) contribute to the process of reendothelialization and prevent neointimal formation after vascular injury. The present study was designed to investigate whether the cysteine-rich 61 (CYR61, CCN1), an important matricellular component of local vascular microenvironment, has effect on EPCs differentiation and reendothelialization in response to vascular injury in rat. Following balloon injury, CCN1 was rapidly induced and dynamically changed at vascular lesions. Overexpression of CCN1 by adenovirus (Ad-CCN1) accelerated reendothelialization and inhibited neointimal formation in the early phase (day 14) after vascular injury (p < 0.05), while no effect was shown on day 21. Ad-CCN1 treatment increased the adhering EPCs on the surface of injured vessels on day 7, and the ratio of GFP- and vWF-positive area to the total luminal length on day 14 was 2.3-fold higher in the Ad-CCN1-EPC-transplanted group than in controls. Consistent with these findings, CCN1-stimulated EPC differentiation in vitro and 20 genes were found differentially expressed during CCN1-induced EPC differentiation, including Id1, Vegf-b, Vegf-c, Kdr, Igf-1, Ereg, Tgf, Mdk, Ptn, Timp2, etc. Among them, negative transcriptional regulator Id1 was associated with CCN1 effect on EPC differentiation. Our data suggest that CCN1, from the microenvironment of injured vessels, enhances reendothelialization via a direct action on EPC differentiation, revealing a possible new mechanism underlying the process of vascular repair.
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页码:713 / 724
页数:11
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