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高分辨率定量计算机断层扫描显示胎盘生长因子-1对小鼠缺血后肢中尺寸侧支血管的选择性增强作用。

High-resolution quantitative computed tomography demonstrating selective enhancement of medium-size collaterals by placental growth factor-1 in the mouse ischemic hindlimb.

作者信息

Li Weiming, Shen Weiqun, Gill Robert, Corbly Angela, Jones Bonita, Belagaje Rama, Zhang Yuke, Tang Shaoqing, Chen Yan, Zhai Yan, Wang Guoming, Wagle Asavari, Hui Kwan, Westmore Michael, Hanson Jeffrey, Chen Yun-Fei, Simons Michael, Singh JaiPal

机构信息

Eli Lilly and Co, Indianapolis, IN 46285, USA.

出版信息

Circulation. 2006 May 23;113(20):2445-53. doi: 10.1161/CIRCULATIONAHA.105.586818. Epub 2006 May 15.

DOI:10.1161/CIRCULATIONAHA.105.586818
PMID:16702473
Abstract

BACKGROUND

The process of arteriogenesis after occlusion of a major artery is poorly understood. We have used high-resolution microcomputed tomography (mu-CT) imaging to define the arteriogenic response in the mouse model of hindlimb ischemia and to examine the effect of placental growth factor-1 (PlGF-1) on this process.

METHODS AND RESULTS

After common femoral artery ligation, mu-CT imaging demonstrated formation of collateral vessels originating near the ligation site in the upper limb and connecting to the ischemic calf muscle region. Three-dimensional mu-CT and quantitative image analysis revealed changes in the number of segments and the segmental volume of vessels, ranging from 8 to 160 microm in diameter. The medium-size vessels (48 to 160 microm) comprising 85% of the vascular volume were the major contributor (188%) to the change in vascular volume in response to ischemia. Intramuscular injections of Ad-PlGF-1 significantly increased Sca1+ cells in the circulation, alpha-actin-stained vessels, and perfusion of the ischemic hindlimb. These effects were predominantly associated with an increase in vascular volume contributed by the medium-size (96 to 144 microm) vessels as determined by mu-CT.

CONCLUSIONS

High-resolution mu-CT delineated the formation of medium-size collaterals representing a major vascular change that contributed to the restoration of vascular volume after ischemia. This effect is selectively potentiated by PlGF-1. Such selective enhancement of arteriogenesis by therapeutically administered PlGF-1 demonstrates a desirable biological activity for promoting the growth of functionally relevant vasculature.

摘要

背景

大动脉闭塞后动脉生成的过程尚不清楚。我们使用高分辨率微型计算机断层扫描(μ-CT)成像来确定后肢缺血小鼠模型中的动脉生成反应,并研究胎盘生长因子-1(PlGF-1)对该过程的影响。

方法与结果

在股总动脉结扎后,μ-CT成像显示在上肢结扎部位附近形成侧支血管,并连接到缺血的小腿肌肉区域。三维μ-CT和定量图像分析显示,直径在8至160微米范围内的血管节段数量和节段体积发生了变化。占血管体积85%的中尺寸血管(48至160微米)是缺血后血管体积变化的主要贡献者(188%)。肌肉注射Ad-PlGF-1显著增加了循环中的Sca1+细胞、α-肌动蛋白染色的血管以及缺血后肢的灌注。这些作用主要与μ-CT测定的中尺寸(96至144微米)血管贡献的血管体积增加有关。

结论

高分辨率μ-CT描绘了中尺寸侧支血管的形成,这是缺血后血管体积恢复的主要血管变化。PlGF-1选择性地增强了这种作用。通过治疗性给予PlGF-1对动脉生成的这种选择性增强显示了促进功能相关脉管系统生长的理想生物学活性。

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